
Review Article

Bone morphogenetic protein signalling in
pulmonary arterial hypertension: revisiting the
BMPRII connection
Wei Li and Kate Quigley

VPD Heart and Lung Research Institute, Department of Medicine, University of Cambridge School of Clinical Medicine, Cambridge CB2 0BB, U.K.

Correspondence: Wei Li(wl225@cam.ac.uk)

Pulmonary arterial hypertension (PAH) is a rare and life-threatening vascular disorder,
characterised by abnormal remodelling of the pulmonary vessels and elevated pulmonary
artery pressure, leading to right ventricular hypertrophy and right-sided heart failure. The
importance of bone morphogenetic protein (BMP) signalling in the pathogenesis of PAH
is demonstrated by human genetic studies. Many PAH risk genes are involved in the
BMP signalling pathway and are highly expressed or preferentially act on vascular endo-
thelial cells. Endothelial dysfunction is recognised as an initial trigger for PAH, and endo-
thelial BMP signalling plays a crucial role in the maintenance of endothelial integrity.
BMPR2 is the most prevalent PAH gene, found in over 80% of heritable cases. As
BMPRII protein is the major type II receptor for a large family of BMP ligands and
expressed ubiquitously in many tissues, dysregulated BMP signalling in other cells may
also contribute to PAH pathobiology. Sotatercept, which contains the extracellular
domain of another transforming growth factor-β family type II receptor ActRIIA fused to
immunoglobin Fc domain, was recently approved by the FDA as a treatment for PAH.
Neither its target cells nor its mechanism of action is fully understood. This review will
revisit BMPRII function and its extracellular regulation, summarise how dysregulated BMP
signalling in endothelial cells and smooth muscle cells may contribute to PAH pathogen-
esis, and discuss how novel therapeutics targeting the extracellular regulation of BMP
signalling, such as BMP9 and Sotatercept, can be related to restoring BMPRII function.

Pulmonary arterial hypertension and bone
morphogenetic protein signalling
Pulmonary arterial hypertension (PAH) is a rare but debilitating condition with a high mortality rate,
affecting 15–26 people per million of the population in western countries [1,2]. The pathology is char-
acterised by the abnormal muscularisation of pre-capillary pulmonary arteries, formation of concen-
tric and plexiform lesions and narrowing of the pulmonary vascular lumen, resulting in an increase in
pulmonary vascular resistance, elevated pulmonary artery pressure, right ventricle hypertrophy, and
progressive right heart failure [3]. The FDA approved PAH therapies prior to 2024 target three path-
ways that predominantly affect vascular tone: endothelin 1, nitric oxide and prostacyclin. Although
these therapies have improved exercise capacity and delayed clinical worsening time, they do not
provide a cure for most patients and survival at three years post-diagnosis remains unacceptably low
[4]. Therapies directly targeting the underlying disease pathophysiology are urgently needed.
Genetic studies suggest that PAH can be caused by pathogenic germline mutations. The most

prevalent disease gene is BMPR2 (bone morphogenetic protein (BMP) receptor 2) [5,6], encoding the
type II receptor for the large family of BMP ligands. BMPR2 mutations are found in over 80% of
familial cases and ∼17% of idiopathic PAH (IPAH) patients [7–9]. Among the 12 validated PAH

Version of Record published:
8 May 2024

Received: 4 March 2024
Revised: 25 April 2024
Accepted: 26 April 2024

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY). 1515

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

http://orcid.org/0000-0002-1924-3120
https://creativecommons.org/licenses/by/4.0/


genes that have been recognised by the International Consortium for Genetic Studies in PAH [10], many are
related to BMP signalling. Apart from BMPR2, ACVRL1 encodes BMP type I receptor activin receptor-like
kinase 1 (ALK1), ENG encodes co-receptor endoglin, GDF2 encodes ligand BMP9, and SMAD9 is a component
of BMP signalling machinery [6,11]. Of note, mutations in PAH genes are predisposing factors with incomplete
penetrance. BMPR2 variants penetrance is estimated to be 42% for heterozygous women and 14% for heterozy-
gous men [6,12].

Introduction to BMP signalling
BMPs are members of the transforming growth factor-β (TGF-β) superfamily. These ligands are mostly homo-
dimers, initiating cellular signalling by forming a complex with cell surface receptors comprising two copies of
a type I receptor and two copies of a type II receptor. Both types of receptors are serine/threonine kinases.
After formation of the signalling complex, the constitutively active type II receptor will phosphorylate and acti-
vate the type I receptor, which will in turn phosphorylate the receptor-regulated SMADs (R-SMADs, including
SMAD1, SMAD5, SMAD9, SMAD2 and SMAD3). The phosphorylated R-SMADs then form a complex with
the common mediator SMAD, SMAD4, and translocate to the nucleus to regulate gene expression. Typically,
BMP signals are mediated by SMAD1, SMAD5 and SMAD9, whereas signals from TGF-βs, Nodal, activins and
some growth and differentiation factors (GDFs) are mediated by SMAD2 and SMAD3. Signalling from the
TGF-β family ligands can also involve non-SMAD pathways such as p38, ERK1/2 and PI3K which impact on
cell proliferation, apoptosis and migration [13]. A more comprehensive review on TGF-β family signalling has
been published recently [14].
TGF-β family ligands are encoded by a total of 33 genes in humans, yet there are only 7 type I and 5 type II

receptors mediating their signals, hence there is a high degree of promiscuity in ligand-receptor interactions.
One BMP ligand can signal via different type I and type II receptor pairs, and the same type I and type II
receptor pair can mediate signals from different ligands. In addition to ligand-receptor interaction, each ligand
is synthesised and secreted as a prodomain bound complex; the prodomain may modify ligand bioactivity or
localisation [15,16]. The extracellular regulation of BMP signalling also involves ligand traps (inhibitors) which
limit ligand availability to the receptors, and cell surface co-receptors (also called type III receptors) which can
modify ligand-receptor interactions [11]. Therefore, the overall signalling outcome is highly context dependent
and determined by local concentrations of different ligands, ligand traps, and cell surface receptors and
co-receptors [17] (Figure 1).
TGF-β and BMP signalling are also regulated at intracellular levels. Inhibitory SMADs, such as SMAD6 and

SMAD7, are target genes of many ligands and can directly inhibit BMP and TGF-β signalling. Some BMPs also
regulate the expression of their own receptors and co-receptors, for example, BMP9 and BMP10 induce the
expression of BMPR2, ENG, SMAD9, and suppress SMAD1 expression in endothelial cells (Figure 1). Such
intracellular regulation provides feedback loops, ensuring a highly dynamic yet tightly controlled BMP signal-
ling outcome.
With such complex regulation mechanisms, it is essential to establish how mutations in different genes lead

to the dysregulated BMP signalling and contribute to the pathobiology of PAH. In addition, it is essential to
understand how BMPR2 mutations might affect signals from different TGF-β family ligands and in different
cell types, which could contribute to the initiation or exacerbation of PAH.

Dysregulated endothelial BMP signalling in the
pathogenesis of PAH
Genetic findings strongly support the crucial role of dysregulated endothelial BMP signalling in the initiation of
PAH. Several genes that are mutated in PAH encode proteins that are part of BMP signalling complex and
highly expressed in vascular endothelial cells, such as BMPR2, ACVRL1 and ENG. Importantly, ACVRL1 is
almost exclusively expressed in endothelial cells, mediating signals from two specific ligands, BMP9 and
BMP10. Mutations in both GDF2 (encoding BMP9) and BMP10 have been identified in PAH patients. The
clinical phenotypes of PAH patients with GDF2 and BMP10 mutations have been characterised in a recent
report [18].
Endothelial dysfunction, which includes endothelial cell apoptosis, compromised barrier function, and altered

vasoactive mediator release, etc, plays a central role in the initiation of PAH [19]. Reduced or loss of endothelial
BMPR2 expression leads to endothelial dysfunction. In vitro, a reduction or loss of BMPR2 in human pulmonary

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY).1516

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


vascular endothelial cells induces mitochondrial dysfunction and promotes a pro-inflammatory and
pro-apoptotic state [20], causes endothelial-to-mesenchymal transition [21], and induces apoptosis [22,23] and
excess permeability [22,24]. BMPRII deficiency impairs apoptosis via the BMPRII-ALK1-BclX (B-cell lymphoma
X)-mediated pathway and the Bcl-xL isoform could be a potential biomarker for PAH [25]. In vivo, loss of

Figure 1. Introduction to the highly dynamic TGF-β and BMP signalling.

TGF-β family signalling is regulated at multiple levels including: (1) TGF-β family ligands are synthesised and secreted as the

prodomain bound forms; (2) there are a large number of ligands signalling through a limited number of type I and type II

receptor pairs with a high degree of promiscuity in ligand-receptor interaction; (3) extracellular ligand traps can bind ligands

and prevent them from binding to the receptors; (4) co-receptors can modify ligand-receptor interactions through direct

protein-protein interactions; (5) TGF-β and BMP signalling can regulate the gene expression of components on the signalling

pathways, such as SMAD9, BMPR2 and ENG, or inhibitors of the signalling pathways, such as SMAD6 and SMAD7. Genes

(and encoded proteins) that are mutated in PAH are highlighted by *.

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY). 1517

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


Bmpr2 causes increased lung vascular permeability [22]. Conditional deletion of Bmpr2 in the pulmonary endo-
thelium [26] or knocking-in human mutation R899X into Bmpr2 gene [22] predisposes mice to PAH.
Circulating BMP ligands, mostly BMP9 and BMP10, act constitutively and potently on vascular endothelial cells
[27,28], inducing BMPR2 expression [29] and have a plethora of endothelial protective functions, including anti-
apoptosis, anti-migration, anti-proliferation, and anti-angiogenesis [22]. Administration of BMP9 neutralising
antibody in adult mice leads to excess permeability in lung vasculature [30].

Crystal structures of the BMPRII signalling complex reveal
the highly dynamic interaction between BMP10 and BMPRII
Although BMPR2 mutations in PAH were first published in 2000, structural insights into how BMPRII inter-
acts with a BMP ligand were only reported in 2022 [31]. Crystal structures of BMPRII extracellular domain
(ECD) in complex with BMP10, and in complex with both BMP10 and ALK1 ECD, revealed an unprecedented
degree of plasticity in the BMPRII:BMP10 interaction [31]. This suggests that stabilising the interaction
between BMPRII and BMP10 requires high concentrations of BMPRII, and that under normal physiological
conditions, BMPRII-dependent signalling is most active in tissues with the highest BMPR2 expression. As lung
vascular endothelial cells have the highest expression of BMPR2, along with the high expression of BMP10 in
the right atrium, together they partly explain why BMPR2 mutations which cause haploinsufficiency will have
the most impact on lung vasculature [31].

BMPR2 mutations also cause dysregulated BMP signalling
in pulmonary smooth muscle cells
BMPRII is the type II receptor for all BMPs, and ubiquitously expressed in many cell types. Germline muta-
tions in BMPR2 also affect its expression in non-endothelial cells. In pulmonary artery smooth muscle cells
(PASMCs) isolated from PAH patients harbouring BMPR2 mutations, BMP4-induced SMAD1 phosphorylation
and ID1 gene expression were reduced [32,33]. The growth suppressive response to BMP4 was lost in proximal
PASMCs harbouring BMPR2 mutations [32].
BMP6 and BMP7 also signal in PASMCs. In one study, it was shown that the induction of ID1 and ID3

gene expression by BMP6 treatment was reduced in BMPR2 mutant PASMCs [33], In another report, the
result was more complicated [34]. In this latter study using mouse Bmpr2−/− and Bmpr2+/− PASMCs, it was
shown that while BMP7 signalling was reduced in Bmpr2+/− PASMCs, there was a gain of BMP6 and BMP7
signalling in Bmpr2−/− PASMCs, even when BMP2 and BMP4 signalling remained reduced upon complete
knockout of Bmpr2. This suggests that after a threshold change of cell surface BMPRII to somewhere below
50%, BMP6 and BMP7 gain of signal appears. More interestingly, in these Bmpr2−/− PASMCs, ActRIIA took
over to mediate BMP4 and BMP6 signalling, and the type I receptor preference changed. ActRIIA can pair up
with both ALK2 and ALK3 to mediate BMP4 signalling in Bmpr2−/− cells, whereas BMP6 (or BMP7) employs
ALK2 only when BMPRII is absent [34]. Such gain of BMP6 signalling was also observed in PASMCs when
BMPRII was shed from cell surface and BMPR2 mRNA levels were reduced by more than 50% upon tumour
necrosis factor-α (TNF-α) treatment [35].

Altered inflammatory response exacerbates loss of BMPRII
function and contributes to PAH pathogenesis
The penetrance of gene mutations causing PAH is low, and a second hit is often present in the pathogenesis of
PAH. Inflammation is widely accepted as a major second hit for PAH, and multiple studies have shown inflam-
mation further contributes to dysregulated BMP signalling in pulmonary vascular cells. BMPRII deficiency pro-
motes an exaggerated inflammatory response in human and mouse SMCs, producing higher levels of IL-6 and
IL-8 after LPS-stimulation compared with controls [36]. TNF-α causes reduced mRNA expression of BMPR2
in both human pulmonary artery endothelial cells (hPAECs) and PASMCs [35], thus exacerbating the loss of
BMPRII protein function in these vascular cells. BMPR2 deficiency in PASMCs conferred insensitivity to
TGF-β induced growth inhibition, and this process is associated with enhanced IL-6 and IL-8 induction by
TGF-β [37]. IL1-β drives an exaggerated inflammatory response when BMPR2 is deficient in PASMCs [38]. On
the endothelial cell front, loss of BMPR2 leads to increased permeability in PAEC monolayers [24], and mice
with an endothelial-specific knockout of Bmpr2 showed increased leukocyte recruitment and reduced barrier

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY).1518

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


function [39]. In humans, aberrant immune regulation is a key feature in a significant proportion of patients
with IPAH and associated with clinical outcomes, with a small subset of patients showing immunoglobin
reactivity to BMPRII [40].

Therapeutic strategies targeting BMP signalling in PAH
There are many ongoing efforts targeting BMP signalling for PAH treatment which have been reviewed recently
[41–44]. Some focus on directly enhancing the cell surface BMPRII expression and such efforts include: (1) ata-
luren/PTC124 which promotes the read-through of stop-gain BMPR2 mutations [45,46]; (2) small chemical
chaperons such as 4-phenylbutyrate (4BA) which promote the secretion of misfolded BMPRII mutant proteins
trapped in the endoplasmic reticulum [47]; (3) chloroquine and hydroxychloroquine which prevent lysosomal
degradation of wild type BMPRII proteins [48]. However, these approaches are not specific to BMPRII, and the
efficacy and potential side effects for treating PAH are yet to be seen in humans. Another approach employs
low-dose FK506 which enhanced BMP signalling and reversed PAH in rodent models [49]. FK506 binds to
FKBP12 and releases it from BMP type I receptors thereby enhancing BMP signalling. In a Phase IIa rando-
mised placebo-controlled trial, FK506 was shown to be safe, increased BMPR2 expression and improved 6-min
walk distance in a subset of patients, but the overall efficacy is yet to be evaluated in a larger, multicentre trial
[50]. Two approaches will be discussed further here: (1) targeting BMP9 signalling, and (2) Sotatercept, which
has been approved by the FDA in March 2024 for treating PAH. Both approaches target the extracellular regu-
lation of the TGF-β family signalling complex.

Targeting BMP9 signalling in PAH and controversies over
BMP9 signalling
Genetic and clinical evidence strongly supports that loss of BMP9 signalling contributes to the pathogenesis of
PAH. Rare heterozygous detrimental mutations in GDF2 (encoding BMP9) have been found in several large
cohort genomic studies [51–53]. Patients with pathogenic BMP9 mutations have lower plasma levels of BMP9
and BMP10 [52,54]. Several homozygous null mutations in GDF2 have also been identified in paediatric PAH
patients and circulating BMP9 is unmeasurable in these patients [54–57].
BMP9 is secreted from the liver and circulates at active concentrations, acting constitutively on vascular

endothelium as a vascular quiescence factor [27]. BMP9 and BMP10 are the only two known high affinity
ligands for ALK1. They form a signalling complex with ALK1 and BMPRII in endothelial cells and signal
potently with an EC50 below 0.1 ng/ml [30,58]. While BMPRII protein levels in endothelial cells reduce rapidly
after protein synthesis inhibition [59], BMP9 induces BMPR2 mRNA expression in endothelial cells [29], thus
forming a dynamic balance. Based on the hypothesis that the loss of endothelial BMPRII and circulating BMP9
could be rescued by supplementation of BMP9, it was reported in 2015 that administration of recombinant
BMP9 reversed PAH in three different rodent models: a genetic mouse knock-in model containing a human
BMPR2 mutation, the monocrotaline (MCT) — induced rat model, and a rat model induced by Sugen along-
side chronic hypoxia (Sugen-Hypoxia) [22]. Here, BMP9 was also shown to confer protection against endothe-
lial dysfunction. For example, in vitro, treatment of hPAECs with BMP9 offered protection against apoptosis
induced by TNF-α and cycloheximide co-treatment, and BMP9 prevented excessive permeability in PAEC
monolayer induced by TNF-α or LPS [22]. Of note, a potential beneficial role of BMP9 has also been reported
in sepsis. Human patients with sepsis have lower BMP9 concentrations at admission, and lower BMP9 concen-
trations are associated with higher risk of death. BMP9 treatment improved the outcome in mice with experi-
mental sepsis [60].
However, Tu et al. [61] reported in 2019 that BMP9 knockout mice, or mice administrated with a neutralis-

ing anti-BMP9 antibody, were significantly protected against chronic hypoxia-induced pulmonary hyperten-
sion. Furthermore, they showed that ALK1-Fc treatment rescued rat PAH models induced either by MCT or
Sugen-Hypoxia. Such results are intriguing as they are different from hypotheses derived from human genetics.
Further studies using BMP9 and BMP10 double knockout mice revealed even more complex picture where the
double knockout mice developed high-output heart failure [62]. Here they also showed that BMP9 contributed
to the hypoxia-induced pulmonary vascular remodelling, whereas BMP10 played a role in hypoxia-induced
cardiac remodelling. In a separate study, BMP9 and BMP10 were shown to directly act on vascular smooth
muscle cells and affect the contractility state of the SMCs [63]. Table 1 summarises in vivo studies supporting
BMP9 agonist or antagonist approaches in the context of PAH.

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY). 1519

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


The controversial observations on BMP9 extend to in vitro cell biological studies. A recent report suggests
that loss of endothelial BMPR2 expression reverses the endothelial response to BMP9, causing enhanced prolif-
eration [65]. It is difficult to compare this study with previous published data as it uses very different treatment
conditions, i.e. 1 ng/ml of BMP9 treatment which is well above the concentrations measured in human plasma
[54], and the experiments were performed in full growth media which already contain high concentrations of
BMP9. Of note, most of the reports use serum-restricted conditions when evaluating BMP9 signalling. Altered
BMP9 response in endothelial cells derived from PAH patients was also observed in another study. Here BMP9

Table 1. Summary of in vivo studies related to BMP9 agonist and antagonist approaches in PAH preclinical models

PMID Journal, year Title of paper, reference number

Key findings related to BMP9
agonist or antagonist approaches in
PAH models

26076038 Nat. Med., 2015 Selective enhancement of endothelial
BMPR-II with BMP9 reverses
pulmonary arterial hypertension [22]

Administration of recombinant BMP9
reversed established PAH in Bmpr2
R899X knock-in mice, as well as in rat
PAH models induced by monocrotaline
or Sugen-Hypoxia.

30636542 Circ. Res., 2019 Selective BMP-9 inhibition partially
protects against experimental
pulmonary hypertension [61]

• Bmp9−/− mice and its inhibition in
C57BL/6 mice using neutralising
anti-BMP9 antibodies substantially
prevent against chronic
hypoxia-induced pulmonary
hypertension.

• The BMP9/BMP10 ligand trap ALK1
ECD administered in monocrotaline or
Sugen/Hypoxia (SuHx) rats
substantially attenuates proliferation of
pulmonary vascular cells,
inflammatory cell infiltration, and
regresses established pulmonary
hypertension in rats.

30312106 Am. J. Respir. Crit.
Care Med., 2019

Bone morphogenetic protein 9 is a
mechanistic biomarker of
portopulmonary hypertension [64]

• Administration of BMP9 ligand trap
ALK1-Fc exacerbated pulmonary
hypertension and pulmonary vascular
remodelling in mice treated with
hypoxia.

33334130 Circulation, 2021 BMP9 and BMP10 act directly on
vascular smooth muscle cells for
generation and maintenance of the
contractile state [63]

• BMP9 KO/BMP10 iKO in right atrium:
dramatic changes in vascular tone
and diminution of the VSMC layer with
attenuated contractility and decreased
systemic as well as right ventricular
systolic pressure.

• Deletion of Acvrl1 (encoding Alk1) in
VSMCs recapitulated the Bmp9/10
phenotype in pulmonary but not in
aortic and coronary arteries.

34086873 Cardiovasc. Res.,
2022

Different cardiovascular and pulmonary
phenotypes for single- and
double-knock-out mice deficient in
BMP9 and BMP10 [62]

• BMP9 contributes to chronic
hypoxia-induced pulmonary vascular
remodelling, whereas BMP10 plays a
role in hypoxia-induced cardiac
remodelling in mice.

• Combined deficiency in Bmp9 and
Bmp10 led to vascular defects
resulting in a decrease in peripheral
vascular resistance and blood
pressure and the progressive
development of high-output heart
failure and pulmonary hemosiderosis.

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY).1520

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


induced unfavourable endothelial-to-mesenchymal transition only in endothelial cells isolated from PAH
patients but not healthy controls [66].
With the current understanding of BMP9 and BMP10 signalling [67,68], it is difficult to reconcile these con-

troversial observations. The functions of BMP9 and BMP10 may have more complexity than hitherto recog-
nised, i.e. more cell types might be involved when investigating BMP9 and BMP10 effects in vivo. One might
interpret such controversial findings as BMP9 exerts different roles at different stages of PAH; a beneficial role
during the initial stage of PAH (where genetic studies are very powerful in identifying the underlying cause of
the disease) and a more complicated role during the late stage of the disease which can often be demonstrated
in cells isolated from patients who are at advanced stages of PAH. Such a scenario was seen for TGF-β, where
it could act as either a tumour suppressor or a tumour promotor depending on different stages of the tumour
development [69].

Sotatercept and ActRIIA-mediated signalling
Sotatercept, a fusion protein comprising the extracellular ligand binding domain of ActRIIA fused to the
Immunoglobin Fc domain, is approved by the FDA for treating Group 1 PAH and is the first PAH therapy tar-
geting the TGF-β superfamily. In a Phase III clinical trial for PAH [70], Sotatercept improved the 6-min walk
distance primary endpoint as well as in eight out of nine secondary efficacy endpoints compared with placebo
controls, including time to death and clinical worsening [70,71]. Adverse events include epistaxis, telangiectasia,
increased haemoglobin levels, thrombocytopenia and increased blood pressure, some of which may be related
to the known affinity of ActRII-A with BMP and GDF ligands.
The mechanism of action of Sotatercept is still not fully understood. An early study suggests that it restores

the balance between SMAD1/5/9 and SMAD2/3 signalling in PAH [72]. Here the authors showed that treat-
ment with ActRIIA-Fc reversed elevated phospho-SMAD2/3 in a rat MCT model, but no restoration of
reduced phospho-SMAD1/5/9 was observed in either rat MCT or rat Sugen-Hypoxia models [72]. Of note,
Sotatercept is a ligand trap for activins and potentially also BMP9 and BMP10, so increased phospho-SMAD1/
5/9 is not a direct outcome expected from Sotatercept treatment. Another study showed that treatment of
ActRIIA-Fc in a Sugen-Hypoxia rat model normalised inflammatory response in the lungs, and importantly,
the treatment suppressed the elevation of Inhba (encoding activin A, or ActA) and Inhbb (encoding ActB)
expression in the right ventricle of Sugen-Hypoxia rats [73]. However, Sotatercept is an extracellular ligand trap
and SMAD proteins are the intracellular mediators of signalling; these data still do not reveal the mode of
action of Sotatercept at direct protein-protein interaction levels. We still do not know which target ligand or
ligands are trapped by Sotatercept for its efficacy in PAH, nor do we know the major cell type that is respon-
sible for the efficacy of Sotatercept.
Ligands with high affinities for ActRIIA are more likely to be bound and inhibited by Sotatercept. ActRIIA

and ActRIIB are the major type II receptors for Activins, and ActRIIA has been shown to mediate signals from
multiple BMP ligands using siRNA approaches [29,34,74]. In Biacore direct binding assays, ActRIIA-Fc has
been shown to bind multiple TGF-β family ligands with high affinities (Table 2). For activin ligands, ActA and
ActB bind to ActRIIA-Fc with the highest affinity [77,79], whereas ActC only binds to ActRIIA transiently and
no reported data on ActE. ActRIIA-Fc binds tightly to several GDF and BMP ligands, with KD in the sub-
nanomolar range for GDF11 and BMP10, and in the nanomolar range for GDF8, BMP7, BMP4, BMP9 and
BMP6 (Table 2, Figure 2). Interestingly, many of these ligands also bind BMPRII with high affinity (Table 3,
Figure 2); for example, ActB binds to BMPRII-Fc with comparable affinity to BMP10 and stronger than many
other BMP ligands [77,79]. ActA also binds BMPRII-Fc with very high affinity, but weaker than ActB or
BMP10. Serum levels of both ActA and ActB are significantly elevated in PAH patients [84]. INHBA (encoding
ActA) is highly expressed in lung microvascular endothelial cells [85]. PAECs isolated from the lungs of
patients with IPAH synthesised more INHBA mRNA and released more ActA protein into the culture medium
[85]. ActA has been shown to be capable of inhibiting BMP9 but not BMP2 and BMP4 signalling in two mul-
tiple myeloma cell lines [86], but such inhibition was not observed in endothelial cells [87]. Interestingly, it was
suggested that BMPRII inhibits activin signalling via ALK2 because knocking down BMPR2 by siRNA lead to
enhanced ActA-phospho-SMAD1/5 signalling via ALK2 in multiple myeloma cells [88]. This observation
agrees with another report that ActA forms a non-signalling complex with ALK2 and type II Activin/BMP
receptors [89]. Taken together, these reports could potentially point to a hypothesis that elevated ActA and
ActB contribute to the disease progression of PAH, partly by competitive binding to BMPRII thereby further
reducing the availability of BMPRII for BMP signalling and exacerbating BMPRII loss. Another potential

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY). 1521

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


mechanism suggested by a recent report is that binding of ActA to BMPRII leads to endocytosis of BMPRII
protein, hence further reducing the cell surface BMPRII [85]. However, increased BMPRII levels or
BMPRII-mediated signalling after ActRIIA-Fc or Sotatercept treatment has not been reported in either preclin-
ical or clinical data. Nevertheless, both hypotheses predict that Sotatercept should have a beneficial effect in
PAH by directly sequestering the elevated ActA and ActB. Of interest, treatment of PAECs with either BMP9
or BMP10, both in the physiologically relevant prodomain-bound forms and at physiologically relevant

Figure 2. Summary of different ligand binding affinities for ActRIIA and BMPRII.

Ligands with high to low affinities for ActRIIA-Fc (A) and BMPRII-Fc (B), based on the binding data in Table 2 and Table 3.

KD values for the high and low affinities are taken from Table 2 and Table 3.

Table 2. Affinities of different ligands for ActRIIA measured by surface
plasmon resonance (Biacore)

Ligands Dissociation constant (KD) and reference paper

ActA 22 pM [75], 23 pM [76], 43 pM [77]a, 59 pM [78]b, 90 pM [79]a

ActB 9.5 pM [75], 61 pM [77]a, 53 pM [79]a

ActC Transient binding [75]

ActE No report

GDF8 3.77 nM [77]a

GDF11 573 pM [77]a, 52 pM [79]a

BMP2 38 nM [78]b, 20.6 nM [80]c, ∼68 nM [81]b

BMP4 ∼3 nM [82], 3.51 nM [77]a, 11.9 nM [80]c

BMP6 10.5 nM [77]a

BMP7 1.59 nM [77]a, 1.2 nM [78]b, No binding [79]a

BMP9 6.43 nM [83]c (25°C)

BMP10 88.6 pM [83] (25°C), 381 pM [77], 1 nM [79]a

Data were obtained using human ActRIIA-Fc immobilised on the Biacore chip and
titrating a range of ligand concentrations apart from those specified in the footnotes
below. Data using immobilised ligands are not included here. Although it is difficult to
directly compare the exact KD values from different studies, the reported values are in
general agreement, and the values obtained from the same study under the same
conditions are directly comparable.aFrom single injection on Biacore.
bUsed mouse ActRIIA, and not Fc fusion.
cBy Steady-state analysis.

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY).1522

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


concentrations, can supress the expression of the INHBB gene which encodes ActB (Figure 3) [90], in agree-
ment with a beneficial effect of a BMP9 agonist approach for treating PAH.

Summary and future directions
Human genetics and pre-clinical studies both support a fundamental role of BMP signalling in the pathogenesis
of PAH. BMP and activin signalling complexes are intertwined at multiple levels, involving the competitive
binding of all three BMP type II receptors, BMPRII, ActRIIA and ActRIIB. The positive outcome from the

Table 3. Affinities of different ligands for BMPRII measured by
surface plasmon resonance (Biacore)

Ligands Dissociation constant (KD) and reference paper

ActA 9.0 nM [77]a, 9.6 nM [79]a

ActB 0.7 nM [79], 0.6 nM [77], 2.3 nM [79]a, 0.7 nM [79]

GDF11 53.3 nM [77]a

BMP2 41.4 [80]b

BMP4 7.4 nM [82], 26.3 nM [80]b

BMP6 44.5 nM [77]a

BMP7 39 nM [77]a, 13 nM [79]a

BMP9 7.4 nM [77]a, 0.6 nM [83]

BMP10 2.4 nM [79], 2.1 nM [79]a, 0.2 nM [77]a, 0.06 nM [83]

Data were obtained using human BMPRII-Fc immobilised on the Biacore chip
and titrating a range of ligand concentrations apart from those specified in the
footnotes below. Data using immobilised ligands are not included here.
Although it is difficult to directly compare the exact KD values from different
studies, the reported values are in general agreement, and the values
obtained from the same study under the same conditions are directly
comparable.aFrom single injection on Biacore.
bBy Steady-state analysis.

Figure 3. BMP9 and BMP10 suppress ActB expression in human pulmonary artery endothelial cells (hPAECs).

Serum-starved hPAECs were treated with PBS, prodomain-bound BMP9 (pro:BMP9), or pro:BMP10 at concentrations

equivalent to 0.4 ng/ml growth factor domain alone. After 5 hours, cells were harvested, and RNA was extracted for microarray

analysis. Volcano plots showing the differential gene expression. Hits with adjusted P values less than 0.05 are shown in red.

INHBB, which encoding ActB, is highlighted. Also highlighted are the components of BMP signalling (Figure 1) that are

regulated by BMP9 and BMP10. Data for PBS vs pro:BMP9 has been published previously [30].

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY). 1523

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


Sotatercept Phase III trial strongly suggests that dysregulated BMP signalling in PAH also involves activin sig-
nalling. A more in-depth investigation of the effect of ActA and ActB in PAH models and patient samples is
warranted. Another area of BMP signalling in PAH that is not covered in this review is the shared mutations of
endothelial BMP signalling components in PAH and hereditary haemorrhagic telangiectasia, which will be
another important and intriguing topic to review.

Perspectives
• The importance of the field: pathogenic mutations in multiple components of BMP signalling

pathways have been identified in human genetic studies on PAH, supporting a crucial role of
dysregulated BMP signalling in the pathogenesis of PAH. Sotatercept is the first
FDA-approved therapeutic modality that directly targets extracellular regulation of TGF-β/BMP
signalling.

• Summary of the current thinking: compromised endothelial BMP signalling involving ALK1 and
BMPRII is likely an initial trigger for PAH. Aberrant BMP signalling in other cell types and other
TGF-β family ligands and receptors may also contribute to the pathogenesis of PAH.

• Future directions: a deeper mechanistic insight into the extracellular regulation of signalling
from BMPs, activins and GDFs may provide novel therapeutic opportunities. This could be
achieved by in vitro cell signalling assays in a physiologically relevant context, such as using
human primary cells, patient cells and co-culture models, and coupled with biochemical and
structural studies to address the direct protein–protein interactions amongst ligands and
receptors.

Competing Interests
The authors declare that there are no competing interests associated with the manuscript.

Funding
W.L. is funded by a British Heart Foundation Senior Basic Science Research Fellowship (FS/SBSRF/20/31005).
K.Q. is funded by British Heart Foundation 4-year PhD programme (FS/4yPhD/F/22/34170C). This research
received support by the NIHR Cambridge Biomedical Research Centre (BRC-1215-20014). The views expressed
are those of the authors and not necessarily those of the NIHR or the Department of Health and Social Care.

Open Access
Open access for this article was enabled by the participation of University of Cambridge in an all-inclusive Read
& Publish agreement with Portland Press and the Biochemical Society under a transformative agreement with
JISC.

Author Contribution
W.L. wrote the manuscript. K.Q. generated Figures 1 and 2 and reviewed the manuscript.

Acknowledgements
We thank Prof. Nick Morrell, Dr Mark Toshner and Dr Jingxu Guo for critically reviewing the manuscript and
providing constructive comments.

Abbreviations
ALK1, activin receptor-like kinase 1; BMP, bone morphogenetic protein; ECD, extracellular domain; GDF, growth
and differentiation factor; hPAEC, human pulmonary artery endothelial cell; IPAH, idiopathic PAH; MCT,
monocrotaline; PAH, pulmonary arterial hypertension; PASMC, pulmonary artery smooth muscle cells; TGF-β,
transforming growth factor-β; TNF-α, tumour necrosis factor-α.

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY).1524

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://creativecommons.org/licenses/by/4.0/


References
1 Humbert, M., Sitbon, O., Chaouat, A., Bertocchi, M., Habib, G., Gressin, V. et al. (2006) Pulmonary arterial hypertension in France: results from a

national registry. Am. J. Respir. Crit. Care Med. 173, 1023–1030 https://doi.org/10.1164/rccm.200510-1668OC
2 Peacock, A.J., Murphy, N.F., McMurray, J.J., Caballero, L. and Stewart, S. (2007) An epidemiological study of pulmonary arterial hypertension. Eur.

Respir. J. 30, 104–109 https://doi.org/10.1183/09031936.00092306
3 Rabinovitch, M. (2012) Molecular pathogenesis of pulmonary arterial hypertension. J. Clin. Invest. 122, 4306–4313 https://doi.org/10.1172/JCI60658
4 Lau, E.M.T., Giannoulatou, E., Celermajer, D.S. and Humbert, M. (2017) Epidemiology and treatment of pulmonary arterial hypertension. Nat. Rev.

Cardiol. 14, 603–614 https://doi.org/10.1038/nrcardio.2017.84
5 Southgate, L., Machado, R.D., Graf, S. and Morrell, N.W. (2020) Molecular genetic framework underlying pulmonary arterial hypertension. Nat. Rev.

Cardiol. 17, 85–95 https://doi.org/10.1038/s41569-019-0242-x
6 Eichstaedt, C.A., Belge, C., Chung, W.K., Graf, S., Grunig, E., Montani, D. et al. (2023) Genetic counselling and testing in pulmonary arterial

hypertension: a consensus statement on behalf of the International Consortium for Genetic Studies in PAH. Eur. Respir. J. 61, 201471 https://doi.org/
10.1183/13993003.01471-2022

7 Evans, J.D., Girerd, B., Montani, D., Wang, X.J., Galie, N., Austin, E.D. et al. (2016) BMPR2 mutations and survival in pulmonary arterial hypertension:
an individual participant data meta-analysis. Lancet Respir. Med. 4, 129–137 https://doi.org/10.1016/S2213-2600(15)00544-5

8 Girerd, B., Montani, D., Jais, X., Eyries, M., Yaici, A., Sztrymf, B. et al. (2016) Genetic counselling in a national referral centre for pulmonary
hypertension. Eur. Respir. J. 47, 541–552 https://doi.org/10.1183/13993003.00717-2015

9 Machado, R.D., Southgate, L., Eichstaedt, C.A., Aldred, M.A., Austin, E.D., Best, D.H. et al. (2015) Pulmonary arterial hypertension: a current
perspective on established and emerging molecular genetic defects. Hum. Mutat. 36, 1113–1127 https://doi.org/10.1002/humu.22904

10 Welch, C.L., Aldred, M.A., Balachandar, S., Dooijes, D., Eichstaedt, C.A., Graf, S. et al. (2023) Defining the clinical validity of genes reported to cause
pulmonary arterial hypertension. Genet Med. 25, 100925 https://doi.org/10.1016/j.gim.2023.100925

11 Li, W., Morrell, N.W. (2022) Endothelial bone morphogenetic protein signaling in pulmonary arterial hypertension. In Encyclopedia of Cell Biology, 2nd
edn, 6, pp. 551–562, ELSEVIER, 2023. https://doi.org/10.1016/B978-0-12-821618-7.00246-7

12 Larkin, E.K, Newman, J.H, Austin, E.D, Hemnes, A.R, Wheeler, L., Robbins, I.M. et al. Longitudinal analysis casts doubt on the presence of genetic
anticipation in heritable pulmonary arterial hypertension. Am. J. Respir. Crit. Care Med. 2012;186:892–896 https://doi.org/10.1164/rccm.
201205-0886OC

13 Al Tabosh, T., Al Tarrass, M., Tourvieilhe, L., Guilhem, A., Dupuis-Girod, S. and Bailly, S. (2024) Hereditary hemorrhagic telangiectasia: from signaling
insights to therapeutic advances. J. Clin. Invest. 134, e176379 https://doi.org/10.1172/JCI176379

14 Miller, D., Hill, C.S. (2023) TGF-β family signaling. In Encyclopedia of Cell Biology, 2nd edn, pp. 46–61, Elsevier, Amsterdam
15 Hinck, A.P., Mueller, T.D. and Springer, T.A. (2016) Structural biology and evolution of the TGF-beta family. Cold Spring Harb. Perspect. Biol. 8,

a022103 https://doi.org/10.1101/cshperspect.a022103
16 Ratcliff, M., Zhou, R.X., Jermutus, L. and Hyvonen, M. (2021) The role of pro-domains in human growth factors and cytokines. Biochem. Soc. Trans.

49, 1963–1973 https://doi.org/10.1042/BST20200663
17 Martinez-Hackert, E., Sundan, A. and Holien, T. (2021) Receptor binding competition: a paradigm for regulating TGF-beta family action. Cytokine Growth

Factor Rev. 57, 39–54 https://doi.org/10.1016/j.cytogfr.2020.09.003
18 Grynblat, J., Bogaard, H.J., Eyries, M., Meyrignac, O., Savale, L., Jais, X. et al. (2024) Pulmonary vascular phenotype identified in patients with GDF2

(BMP9) or BMP10 variants: an international multicentre study. Eur. Respir. J. 63, 2301634 https://doi.org/10.1183/13993003.01634-2023
19 Budhiraja, R., Tuder, R.M. and Hassoun, P.M. (2004) Endothelial dysfunction in pulmonary hypertension. Circulation 109, 159–165 https://doi.org/10.

1161/01.CIR.0000102381.57477.50
20 Diebold, I., Hennigs, J.K., Miyagawa, K., Li, C.G., Nickel, N.P., Kaschwich, M. et al. (2015) BMPR2 preserves mitochondrial function and DNA during

reoxygenation to promote endothelial cell survival and reverse pulmonary hypertension. Cell Metab. 21, 596–608 https://doi.org/10.1016/j.cmet.2015.
03.010

21 Hopper, R.K., Moonen, J.R., Diebold, I., Cao, A., Rhodes, C.J., Tojais, N.F. et al. (2016) In pulmonary arterial hypertension, reduced BMPR2 promotes
endothelial-to-mesenchymal transition via HMGA1 and its target slug. Circulation 133, 1783–1794 https://doi.org/10.1161/CIRCULATIONAHA.115.
020617

22 Long, L., Ormiston, M.L., Yang, X., Southwood, M., Graf, S., Machado, R.D. et al. (2015) Selective enhancement of endothelial BMPR-II with BMP9
reverses pulmonary arterial hypertension. Nat. Med. 21, 777–785 https://doi.org/10.1038/nm.3877

23 Teichert-Kuliszewska, K., Kutryk, M.J., Kuliszewski, M.A., Karoubi, G., Courtman, D.W., Zucco, L. et al. (2006) Bone morphogenetic protein receptor-2
signaling promotes pulmonary arterial endothelial cell survival: implications for loss-of-function mutations in the pathogenesis of pulmonary hypertension.
Circ. Res. 98, 209–217 https://doi.org/10.1161/01.RES.0000200180.01710.e6

24 Burton, V.J., Ciuclan, L.I., Holmes, A.M., Rodman, D.M., Walker, C. and Budd, D.C. (2011) Bone morphogenetic protein receptor II regulates pulmonary
artery endothelial cell barrier function. Blood 117, 333–341 https://doi.org/10.1182/blood-2010-05-285973

25 Chowdhury, H.M., Sharmin, N., Yuzbasioglu Baran, M., Long, L., Morrell, N.W., Trembath, R.C. et al. (2019) BMPRII deficiency impairs apoptosis via the
BMPRII-ALK1-BclX-mediated pathway in pulmonary arterial hypertension. Hum. Mol. Genet. 28, 2161–2173 https://doi.org/10.1093/hmg/ddz047

26 Hong, K.H., Lee, Y.J., Lee, E., Park, S.O., Han, C., Beppu, H. et al. (2008) Genetic ablation of the BMPR2 gene in pulmonary endothelium is sufficient
to predispose to pulmonary arterial hypertension. Circulation 118, 722–730 https://doi.org/10.1161/CIRCULATIONAHA.107.736801

27 Bidart, M., Ricard, N., Levet, S., Samson, M., Mallet, C., David, L. et al. (2012) BMP9 is produced by hepatocytes and circulates mainly in an active
mature form complexed to its prodomain. Cell. Mol. Life Sci. 69, 313–324 https://doi.org/10.1007/s00018-011-0751-1

28 Jiang, H., Salmon, R.M., Upton, P.D., Wei, Z., Lawera, A., Davenport, A.P. et al. (2016) The prodomain-bound form of bone morphogenetic protein 10
is biologically active on endothelial cells. J. Biol. Chem. 291, 2954–2966 https://doi.org/10.1074/jbc.M115.683292

29 Upton, P.D., Davies, R.J., Trembath, R.C. and Morrell, N.W. (2009) Bone morphogenetic protein (BMP) and activin type II receptors balance BMP9
signals mediated by activin receptor-like kinase-1 in human pulmonary artery endothelial cells. J. Biol. Chem. 284, 15794–15804 https://doi.org/10.
1074/jbc.M109.002881

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY). 1525

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://doi.org/10.1164/rccm.200510-1668OC
https://doi.org/10.1164/rccm.200510-1668OC
https://doi.org/10.1183/09031936.00092306
https://doi.org/10.1172/JCI60658
https://doi.org/10.1038/nrcardio.2017.84
https://doi.org/10.1038/s41569-019-0242-x
https://doi.org/10.1038/s41569-019-0242-x
https://doi.org/10.1038/s41569-019-0242-x
https://doi.org/10.1038/s41569-019-0242-x
https://doi.org/10.1183/13993003.01471-2022
https://doi.org/10.1183/13993003.01471-2022
https://doi.org/10.1183/13993003.01471-2022
https://doi.org/10.1016/S2213-2600(15)00544-5
https://doi.org/10.1016/S2213-2600(15)00544-5
https://doi.org/10.1016/S2213-2600(15)00544-5
https://doi.org/10.1183/13993003.00717-2015
https://doi.org/10.1183/13993003.00717-2015
https://doi.org/10.1002/humu.22904
https://doi.org/10.1016/j.gim.2023.100925
https://doi.org/10.1016/B978-0-12-821618-7.00246-7
https://doi.org/10.1164/rccm.201205-0886OC
https://doi.org/10.1164/rccm.201205-0886OC
https://doi.org/10.1164/rccm.201205-0886OC
https://doi.org/10.1172/JCI176379
https://doi.org/10.1101/cshperspect.a022103
https://doi.org/10.1042/BST20200663
https://doi.org/10.1016/j.cytogfr.2020.09.003
https://doi.org/10.1183/13993003.01634-2023
https://doi.org/10.1183/13993003.01634-2023
https://doi.org/10.1161/01.CIR.0000102381.57477.50
https://doi.org/10.1161/01.CIR.0000102381.57477.50
https://doi.org/10.1016/j.cmet.2015.03.010
https://doi.org/10.1016/j.cmet.2015.03.010
https://doi.org/10.1161/CIRCULATIONAHA.115.020617
https://doi.org/10.1161/CIRCULATIONAHA.115.020617
https://doi.org/10.1038/nm.3877
https://doi.org/10.1161/01.RES.0000200180.01710.e6
https://doi.org/10.1182/blood-2010-05-285973
https://doi.org/10.1182/blood-2010-05-285973
https://doi.org/10.1182/blood-2010-05-285973
https://doi.org/10.1182/blood-2010-05-285973
https://doi.org/10.1093/hmg/ddz047
https://doi.org/10.1161/CIRCULATIONAHA.107.736801
https://doi.org/10.1007/s00018-011-0751-1
https://doi.org/10.1007/s00018-011-0751-1
https://doi.org/10.1007/s00018-011-0751-1
https://doi.org/10.1007/s00018-011-0751-1
https://doi.org/10.1074/jbc.M115.683292
https://doi.org/10.1074/jbc.M109.002881
https://doi.org/10.1074/jbc.M109.002881
https://creativecommons.org/licenses/by/4.0/


30 Li, W., Long, L., Yang, X., Tong, Z., Southwood, M., King, R. et al. (2021) Circulating BMP9 protects the pulmonary endothelium during
inflammation-induced lung injury in mice. Am. J. Respir. Crit. Care Med. 203, 1419–1430 https://doi.org/10.1164/rccm.202005-1761OC

31 Guo, J., Liu, B., Thorikay, M., Yu, M., Li, X., Tong, Z. et al. (2022) Crystal structures of BMPRII extracellular domain in binary and ternary receptor
complexes with BMP10. Nat. Commun. 13, 2395 https://doi.org/10.1038/s41467-022-30111-2

32 Yang, X., Long, L., Southwood, M., Rudarakanchana, N., Upton, P.D., Jeffery, T.K. et al. (2005) Dysfunctional Smad signaling contributes to abnormal
smooth muscle cell proliferation in familial pulmonary arterial hypertension. Circ. Res. 96, 1053–1063 https://doi.org/10.1161/01.RES.0000166926.
54293.68

33 Yang, J., Li, X., Li, Y., Southwood, M., Ye, L., Long, L. et al. (2013) Id proteins are critical downstream effectors of BMP signaling in human pulmonary
arterial smooth muscle cells. Am. J. Physiol. Lung Cell. Mol. Physiol. 305, L312–L321 https://doi.org/10.1152/ajplung.00054.2013

34 Yu, P.B., Beppu, H., Kawai, N., Li, E. and Bloch, K.D. (2005) Bone morphogenetic protein (BMP) type II receptor deletion reveals BMP ligand-specific
gain of signaling in pulmonary artery smooth muscle cells. J. Biol. Chem. 280, 24443–24450 https://doi.org/10.1074/jbc.M502825200

35 Hurst, L.A., Dunmore, B.J., Long, L., Crosby, A., Al-Lamki, R., Deighton, J. et al. (2017) TNFalpha drives pulmonary arterial hypertension by
suppressing the BMP type-II receptor and altering NOTCH signalling. Nat. Commun. 8, 14079 https://doi.org/10.1038/ncomms14079

36 Soon, E., Crosby, A., Southwood, M., Yang, P., Tajsic, T., Toshner, M. et al. (2015) Bone morphogenetic protein receptor type II deficiency and
increased inflammatory cytokine production. A gateway to pulmonary arterial hypertension. Am. J. Respir. Crit. Care Med. 192, 859–872 https://doi.org/
10.1164/rccm.201408-1509OC

37 Davies, R.J., Holmes, A.M., Deighton, J., Long, L., Yang, X., Barker, L. et al. (2012) BMP type II receptor deficiency confers resistance to growth
inhibition by TGF-beta in pulmonary artery smooth muscle cells: role of proinflammatory cytokines. Am. J. Physiol. Lung Cell. Mol. Physiol. 302,
L604–L615 https://doi.org/10.1152/ajplung.00309.2011

38 Pickworth, J., Rothman, A., Iremonger, J., Casbolt, H., Hopkinson, K., Hickey, P.M. et al. (2017) Differential IL-1 signaling induced by BMPR2 deficiency
drives pulmonary vascular remodeling. Pulm. Circ. 7, 768–776 https://doi.org/10.1177/2045893217729096

39 Burton, V.J., Holmes, A.M., Ciuclan, L.I., Robinson, A., Roger, J.S., Jarai, G. et al. (2011) Attenuation of leukocyte recruitment via CXCR1/2 inhibition
stops the progression of PAH in mice with genetic ablation of endothelial BMPR-II. Blood 118, 4750–4758 https://doi.org/10.1182/
blood-2011-05-347393

40 Jones, R.J., De Bie, E., Groves, E., Zalewska, K.I., Swietlik, E.M., Treacy, C.M. et al. (2022) Autoimmunity is a significant feature of idiopathic
pulmonary arterial hypertension. Am. J. Respir. Crit. Care Med. 206, 81–93 https://doi.org/10.1164/rccm.202108-1919OC

41 Sharmin, N., Nganwuchu, C.C. and Nasim, M.T. (2021) Targeting the TGF-beta signaling pathway for resolution of pulmonary arterial hypertension.
Trends Pharmacol. Sci. 42, 510–513 https://doi.org/10.1016/j.tips.2021.04.002

42 Dunmore, B.J., Jones, R.J., Toshner, M.R., Upton, P.D. and Morrell, N.W. (2021) Approaches to treat pulmonary arterial hypertension by targeting
BMPR2: from cell membrane to nucleus. Cardiovasc. Res. 117, 2309–2325 https://doi.org/10.1093/cvr/cvaa350

43 Ali, M.K., Ichimura, K. and Spiekerkoetter, E. (2021) Promising therapeutic approaches in pulmonary arterial hypertension. Curr. Opin. Pharmacol. 59,
127–139 https://doi.org/10.1016/j.coph.2021.05.003

44 Dannewitz Prosseda, S., Ali, M.K. and Spiekerkoetter, E. (2020) Novel advances in modifying BMPR2 signaling in PAH. Genes (Basel) 12, 8 https://doi.
org/10.3390/genes12010008

45 Drake, K.M., Dunmore, B.J., McNelly, L.N., Morrell, N.W. and Aldred, M.A. (2013) Correction of nonsense BMPR2 and SMAD9 mutations by ataluren in
pulmonary arterial hypertension. Am. J. Respir. Cell Mol. Biol. 49, 403–409 https://doi.org/10.1165/rcmb.2013-0100OC

46 Long, L., Yang, X., Southwood, M., Moore, S., Crosby, A., Upton, P.D. et al. (2020) Targeting translational read-through of premature termination
mutations in BMPR2 with PTC124 for pulmonary arterial hypertension. Pulm. Circ. 10, 2045894020935783 https://doi.org/10.1177/
2045894020935783

47 Dunmore, B.J., Yang, X., Crosby, A., Moore, S., Long, L., Huang, C. et al. (2020) 4PBA restores signaling of a cysteine-substituted mutant BMPR2
receptor found in patients with pulmonary arterial hypertension. Am. J. Respir. Cell Mol. Biol. 63, 160–171 https://doi.org/10.1165/rcmb.2019-0321OC

48 Long, L., Yang, X., Southwood, M., Lu, J., Marciniak, S.J., Dunmore, B.J. et al. (2013) Chloroquine prevents progression of experimental pulmonary
hypertension via inhibition of autophagy and lysosomal bone morphogenetic protein type II receptor degradation. Circ. Res. 112, 1159–1170 https://doi.
org/10.1161/CIRCRESAHA.111.300483

49 Spiekerkoetter, E., Tian, X., Cai, J., Hopper, R.K., Sudheendra, D., Li, C.G. et al. (2013) FK506 activates BMPR2, rescues endothelial dysfunction, and
reverses pulmonary hypertension. J. Clin. Invest. 123, 3600–3613 https://doi.org/10.1172/JCI65592

50 Spiekerkoetter, E., Sung, Y.K., Sudheendra, D., Scott, V., Del Rosario, P., Bill, M. et al. (2017) Randomised placebo-controlled safety and tolerability trial
of FK506 (tacrolimus) for pulmonary arterial hypertension. Eur. Respir. J. 50, 1602449 https://doi.org/10.1183/13993003.02449-2016

51 Graf, S., Haimel, M., Bleda, M., Hadinnapola, C., Southgate, L., Li, W. et al. (2018) Identification of rare sequence variation underlying heritable
pulmonary arterial hypertension. Nat. Commun. 9, 1416 https://doi.org/10.1038/s41467-018-03672-4

52 Wang, X.J., Lian, T.Y., Jiang, X., Liu, S.F., Li, S.Q., Jiang, R. et al. (2019) Germline BMP9 mutation causes idiopathic pulmonary arterial hypertension.
Eur. Respir. J. 53, 1801609 https://doi.org/10.1183/13993003.01609-2018

53 Eyries, M., Montani, D., Girerd, B., Favrolt, N., Riou, M., Faivre, L. et al. (2020) Familial pulmonary arterial hypertension by KDR heterozygous loss of
function. Eur. Respir. J. 55, 1902165 https://doi.org/10.1183/13993003.02165-2019

54 Hodgson, J., Ruiz-Llorente, L., McDonald, J., Quarrell, O., Ugonna, K., Bentham, J. et al. (2021) Homozygous GDF2 nonsense mutations result in a loss
of circulating BMP9 and BMP10 and are associated with either PAH or an “HHT-like” syndrome in children. Mol. Genet. Genomic Med. 9, e1685
https://doi.org/10.1002/mgg3.1685

55 Upton, P., Richards, S., Bates, A., Niederhoffer, K.Y., Morrell, N.W. and Christian, S. (2023) A rare homozygous missense GDF2 (BMP9) mutation
causing PAH in siblings: does BMP10 status contribute? Am. J. Med. Genet. A 191, 228–233 https://doi.org/10.1002/ajmg.a.62996

56 Chomette, L., Hupkens, E., Romitti, M., Dewachter, L., Vachiery, J.L., Bailly, S. et al. (2023) Pediatric pulmonary arterial hypertension due to a novel
homozygous GDF2 missense variant affecting BMP9 processing and activity. Am. J. Med. Genet. A 191, 2064–2073 https://doi.org/10.1002/ajmg.a.
63236

57 Wang, G., Fan, R., Ji, R., Zou, W., Penny, D.J., Varghese, N.P. et al. (2016) Novel homozygous BMP9 nonsense mutation causes pulmonary arterial
hypertension: a case report. BMC Pulm. Med. 16, 17 https://doi.org/10.1186/s12890-016-0183-7

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY).1526

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://doi.org/10.1164/rccm.202005-1761OC
https://doi.org/10.1164/rccm.202005-1761OC
https://doi.org/10.1038/s41467-022-30111-2
https://doi.org/10.1038/s41467-022-30111-2
https://doi.org/10.1038/s41467-022-30111-2
https://doi.org/10.1038/s41467-022-30111-2
https://doi.org/10.1161/01.RES.0000166926.54293.68
https://doi.org/10.1161/01.RES.0000166926.54293.68
https://doi.org/10.1152/ajplung.00054.2013
https://doi.org/10.1074/jbc.M502825200
https://doi.org/10.1038/ncomms14079
https://doi.org/10.1164/rccm.201408-1509OC
https://doi.org/10.1164/rccm.201408-1509OC
https://doi.org/10.1164/rccm.201408-1509OC
https://doi.org/10.1152/ajplung.00309.2011
https://doi.org/10.1177/2045893217729096
https://doi.org/10.1182/blood-2011-05-347393
https://doi.org/10.1182/blood-2011-05-347393
https://doi.org/10.1182/blood-2011-05-347393
https://doi.org/10.1182/blood-2011-05-347393
https://doi.org/10.1182/blood-2011-05-347393
https://doi.org/10.1164/rccm.202108-1919OC
https://doi.org/10.1164/rccm.202108-1919OC
https://doi.org/10.1016/j.tips.2021.04.002
https://doi.org/10.1093/cvr/cvaa350
https://doi.org/10.1016/j.coph.2021.05.003
https://doi.org/10.3390/genes12010008
https://doi.org/10.3390/genes12010008
https://doi.org/10.1165/rcmb.2013-0100OC
https://doi.org/10.1165/rcmb.2013-0100OC
https://doi.org/10.1177/2045894020935783
https://doi.org/10.1177/2045894020935783
https://doi.org/10.1165/rcmb.2019-0321OC
https://doi.org/10.1165/rcmb.2019-0321OC
https://doi.org/10.1161/CIRCRESAHA.111.300483
https://doi.org/10.1161/CIRCRESAHA.111.300483
https://doi.org/10.1172/JCI65592
https://doi.org/10.1183/13993003.02449-2016
https://doi.org/10.1183/13993003.02449-2016
https://doi.org/10.1038/s41467-018-03672-4
https://doi.org/10.1038/s41467-018-03672-4
https://doi.org/10.1038/s41467-018-03672-4
https://doi.org/10.1038/s41467-018-03672-4
https://doi.org/10.1183/13993003.01609-2018
https://doi.org/10.1183/13993003.01609-2018
https://doi.org/10.1183/13993003.02165-2019
https://doi.org/10.1183/13993003.02165-2019
https://doi.org/10.1002/mgg3.1685
https://doi.org/10.1002/ajmg.a.62996
https://doi.org/10.1002/ajmg.a.63236
https://doi.org/10.1002/ajmg.a.63236
https://doi.org/10.1186/s12890-016-0183-7
https://doi.org/10.1186/s12890-016-0183-7
https://doi.org/10.1186/s12890-016-0183-7
https://doi.org/10.1186/s12890-016-0183-7
https://creativecommons.org/licenses/by/4.0/


58 David, L., Mallet, C., Keramidas, M., Lamande, N., Gasc, J.M., Dupuis-Girod, S. et al. (2008) Bone morphogenetic protein-9 is a circulating vascular
quiescence factor. Circ. Res. 102, 914–922 https://doi.org/10.1161/CIRCRESAHA.107.165530

59 Dunmore, B.J., Drake, K.M., Upton, P.D., Toshner, M.R., Aldred, M.A. and Morrell, N.W. (2013) The lysosomal inhibitor, chloroquine, increases cell
surface BMPR-II levels and restores BMP9 signalling in endothelial cells harbouring BMPR-II mutations. Hum. Mol. Genet. 22, 3667–3679 https://doi.
org/10.1093/hmg/ddt216

60 Bai, H., Lu, Q., Wu, C., Xu, F., Liu, J., Wang, K. et al. (2024) Bone morphogenetic protein 9 is a candidate prognostic biomarker and host-directed
therapy target for sepsis. Sci. Transl. Med. 16, eadi3275 https://doi.org/10.1126/scitranslmed.adi3275

61 Tu, L., Desroches-Castan, A., Mallet, C., Guyon, L., Cumont, A., Phan, C. et al. (2019) Selective BMP-9 inhibition partially protects against experimental
pulmonary hypertension. Circ. Res. 124, 846–855 https://doi.org/10.1161/CIRCRESAHA.118.313356

62 Bouvard, C., Tu, L., Rossi, M., Desroches-Castan, A., Berrebeh, N., Helfer, E. et al. (2022) Different cardiovascular and pulmonary phenotypes for
single- and double-knock-out mice deficient in BMP9 and BMP10. Cardiovasc. Res. 118, 1805–1820 https://doi.org/10.1093/cvr/cvab187

63 Wang, L., Rice, M., Swist, S., Kubin, T., Wu, F., Wang, S. et al. (2021) BMP9 and BMP10 act directly on vascular smooth muscle cells for generation
and maintenance of the contractile state. Circulation 143, 1394–1410 https://doi.org/10.1161/CIRCULATIONAHA.120.047375

64 Nikolic, I., Yung, L.M., Yang, P., Malhotra, R., Paskin-Flerlage, S.D., Dinter, T. et al. (2019) Bone morphogenetic protein 9 is a mechanistic biomarker of
portopulmonary hypertension. Am. J. Respir. Crit. Care Med. 199, 891–902 https://doi.org/10.1164/rccm.201807-1236OC

65 Theilmann, A.L., Hawke, L.G., Hilton, L.R., Whitford, M.K.M., Cole, D.V., Mackeil, J.L. et al. (2020) Endothelial BMPR2 loss drives a proliferative
response to BMP (bone morphogenetic protein) 9 via prolonged canonical signaling. Arterioscler. Thromb. Vasc. Biol. 40, 2605–2618 https://doi.org/10.
1161/ATVBAHA.119.313357

66 Szulcek, R., Sanchez-Duffhues, G., Rol, N., Pan, X., Tsonaka, R., Dickhoff, C. et al. (2020) Exacerbated inflammatory signaling underlies aberrant
response to BMP9 in pulmonary arterial hypertension lung endothelial cells. Angiogenesis 23, 699–714 https://doi.org/10.1007/s10456-020-09741-x

67 Upton, P.D., Dunmore, B.J., Li, W. and Morrell, N.W. (2022) An emerging class of new therapeutics targeting TGF, Activin, and BMP ligands in
pulmonary arterial hypertension. Dev. Dyn. 252, 327–342 https://doi.org/10.1002/dvdy.478

68 Desroches-Castan, A., Tillet, E., Bouvard, C. and Bailly, S. (2022) BMP9 and BMP10: two close vascular quiescence partners that stand out. Dev. Dyn.
251, 178–197 https://doi.org/10.1002/dvdy.395

69 Massague, J. (2008) TGFbeta in cancer. Cell 134, 215–230 https://doi.org/10.1016/j.cell.2008.07.001
70 Hoeper, M.M., Badesch, D.B., Ghofrani, H.A., Gibbs, J.S.R., Gomberg-Maitland, M., McLaughlin, V.V. et al. (2023) Phase 3 trial of sotatercept for

treatment of pulmonary arterial hypertension. N. Engl. J. Med. 388, 1478–1490 https://doi.org/10.1056/NEJMoa2213558
71 Humbert, M. (2023) Viewpoint: activin signalling inhibitors for the treatment of pulmonary arterial hypertension. Eur. Respir. J. 62, 2301726 https://doi.

org/10.1183/13993003.01726-2023
72 Yung, L.M., Yang, P., Joshi, S., Augur, Z.M., Kim, S.S.J., Bocobo, G.A. et al. (2020) ACTRIIA-Fc rebalances activin/GDF versus BMP signaling in

pulmonary hypertension. Sci. Transl. Med. 12, eaaz5660 https://doi.org/10.1126/scitranslmed.aaz5660
73 Joshi, S.R., Liu, J., Bloom, T., Karaca Atabay, E., Kuo, T.H., Lee, M. et al. (2022) Sotatercept analog suppresses inflammation to reverse experimental

pulmonary arterial hypertension. Sci. Rep. 12, 7803 https://doi.org/10.1038/s41598-022-11435-x
74 David, L., Mallet, C., Mazerbourg, S., Feige, J.J. and Bailly, S. (2007) Identification of BMP9 and BMP10 as functional activators of the orphan activin

receptor-like kinase 1 (ALK1) in endothelial cells. Blood 109, 1953–1961 https://doi.org/10.1182/blood-2006-07-034124
75 Goebel, E.J., Ongaro, L., Kappes, E.C., Vestal, K., Belcheva, E., Castonguay, R. et al. (2022) The orphan ligand, activin C, signals through activin

receptor-like kinase 7. Elife 11, e78197 https://doi.org/10.7554/eLife.78197
76 Aykul, S., Ni, W., Mutatu, W. and Martinez-Hackert, E. (2015) Human Cerberus prevents nodal-receptor binding, inhibits nodal signaling, and suppresses

nodal-mediated phenotypes. PLoS One 10, e0114954 https://doi.org/10.1371/journal.pone.0114954
77 Aykul, S. and Martinez-Hackert, E. (2016) Transforming growth factor-beta family ligands can function as antagonists by competing for type II receptor

binding. J. Biol. Chem. 291, 10792–10804 https://doi.org/10.1074/jbc.M115.713487
78 Greenwald, J., Groppe, J., Gray, P., Wiater, E., Kwiatkowski, W., Vale, W. et al. (2003) The BMP7/ActRII extracellular domain complex provides new

insights into the cooperative nature of receptor assembly. Mol. Cell 11, 605–617 https://doi.org/10.1016/s1097-2765(03)00094-7
79 Chu, K.Y., Malik, A., Thamilselvan, V. and Martinez-Hackert, E. (2022) Type II BMP and activin receptors BMPR2 and ACVR2A share a conserved mode

of growth factor recognition. J. Biol. Chem. 298, 102076 https://doi.org/10.1016/j.jbc.2022.102076
80 Gipson, G.R., Nolan, K., Kattamuri, C., Kenny, A.P., Agricola, Z., Edwards, N.A. et al. (2023) Formation and characterization of BMP2/GDF5 and BMP4/

GDF5 heterodimers. BMC Biol. 21, 16 https://doi.org/10.1186/s12915-023-01522-4
81 Allendorph, G.P., Vale, W.W. and Choe, S. (2006) Structure of the ternary signaling complex of a TGF-beta superfamily member. Proc. Natl Acad. Sci.

U.S.A. 103, 7643–7648 https://doi.org/10.1073/pnas.0602558103
82 Aykul, S. and Martinez-Hackert, E. (2016) Determination of half-maximal inhibitory concentration using biosensor-based protein interaction analysis.

Anal. Biochem. 508, 97–103 https://doi.org/10.1016/j.ab.2016.06.025
83 Townson, S.A., Martinez-Hackert, E., Greppi, C., Lowden, P., Sako, D., Liu, J. et al. (2012) Specificity and structure of a high affinity activin receptor-like

kinase 1 (ALK1) signaling complex. J. Biol. Chem. 287, 27313–27325 https://doi.org/10.1074/jbc.M112.377960
84 Guignabert, C., Savale, L., Boucly, A., Thuillet, R., Tu, L., Ottaviani, M. et al. (2023) Serum and pulmonary expression profiles of the activin signaling

system in pulmonary arterial hypertension. Circulation 147, 1809–1822 https://doi.org/10.1161/CIRCULATIONAHA.122.061501
85 Ryanto, G.R.T., Ikeda, K., Miyagawa, K., Tu, L., Guignabert, C., Humbert, M. et al. (2021) An endothelial activin A-bone morphogenetic protein receptor

type 2 link is overdriven in pulmonary hypertension. Nat. Commun. 12, 1720 https://doi.org/10.1038/s41467-021-21961-3
86 Olsen, O.E., Wader, K.F., Hella, H., Mylin, A.K., Turesson, I., Nesthus, I. et al. (2015) Activin A inhibits BMP-signaling by binding ACVR2A and ACVR2B.

Cell Commun. Signal. 13, 27 https://doi.org/10.1186/s12964-015-0104-z
87 Wood, J.H., Guo, J., Morrell, N.W. and Li, W. (2019) Advances in the molecular regulation of endothelial BMP9 signalling complexes and implications

for cardiovascular disease. Biochem. Soc. Trans. 47, 779–791 https://doi.org/10.1042/BST20180137
88 Olsen, O.E., Sankar, M., Elsaadi, S., Hella, H., Buene, G., Darvekar, S.R. et al. (2018) BMPR2 inhibits activin and BMP signaling via wild-type ALK2.

J. Cell Sci. 131, jcs213512 https://doi.org/10.1242/jcs.213512

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY). 1527

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://doi.org/10.1161/CIRCRESAHA.107.165530
https://doi.org/10.1093/hmg/ddt216
https://doi.org/10.1093/hmg/ddt216
https://doi.org/10.1126/scitranslmed.adi3275
https://doi.org/10.1161/CIRCRESAHA.118.313356
https://doi.org/10.1093/cvr/cvab187
https://doi.org/10.1161/CIRCULATIONAHA.120.047375
https://doi.org/10.1164/rccm.201807-1236OC
https://doi.org/10.1164/rccm.201807-1236OC
https://doi.org/10.1161/ATVBAHA.119.313357
https://doi.org/10.1161/ATVBAHA.119.313357
https://doi.org/10.1007/s10456-020-09741-x
https://doi.org/10.1007/s10456-020-09741-x
https://doi.org/10.1007/s10456-020-09741-x
https://doi.org/10.1007/s10456-020-09741-x
https://doi.org/10.1002/dvdy.478
https://doi.org/10.1002/dvdy.395
https://doi.org/10.1016/j.cell.2008.07.001
https://doi.org/10.1056/NEJMoa2213558
https://doi.org/10.1183/13993003.01726-2023
https://doi.org/10.1183/13993003.01726-2023
https://doi.org/10.1183/13993003.01726-2023
https://doi.org/10.1126/scitranslmed.aaz5660
https://doi.org/10.1038/s41598-022-11435-x
https://doi.org/10.1038/s41598-022-11435-x
https://doi.org/10.1038/s41598-022-11435-x
https://doi.org/10.1038/s41598-022-11435-x
https://doi.org/10.1182/blood-2006-07-034124
https://doi.org/10.1182/blood-2006-07-034124
https://doi.org/10.1182/blood-2006-07-034124
https://doi.org/10.1182/blood-2006-07-034124
https://doi.org/10.7554/eLife.78197
https://doi.org/10.1371/journal.pone.0114954
https://doi.org/10.1074/jbc.M115.713487
https://doi.org/10.1016/s1097-2765(03)00094-7
https://doi.org/10.1016/s1097-2765(03)00094-7
https://doi.org/10.1016/s1097-2765(03)00094-7
https://doi.org/10.1016/j.jbc.2022.102076
https://doi.org/10.1186/s12915-023-01522-4
https://doi.org/10.1186/s12915-023-01522-4
https://doi.org/10.1186/s12915-023-01522-4
https://doi.org/10.1186/s12915-023-01522-4
https://doi.org/10.1073/pnas.0602558103
https://doi.org/10.1016/j.ab.2016.06.025
https://doi.org/10.1074/jbc.M112.377960
https://doi.org/10.1161/CIRCULATIONAHA.122.061501
https://doi.org/10.1038/s41467-021-21961-3
https://doi.org/10.1038/s41467-021-21961-3
https://doi.org/10.1038/s41467-021-21961-3
https://doi.org/10.1038/s41467-021-21961-3
https://doi.org/10.1186/s12964-015-0104-z
https://doi.org/10.1186/s12964-015-0104-z
https://doi.org/10.1186/s12964-015-0104-z
https://doi.org/10.1186/s12964-015-0104-z
https://doi.org/10.1042/BST20180137
https://doi.org/10.1242/jcs.213512
https://creativecommons.org/licenses/by/4.0/


89 Aykul, S., Corpina, R.A., Goebel, E.J., Cunanan, C.J., Dimitriou, A., Kim, H.J. et al. (2020) Activin A forms a non-signaling complex with ACVR1 and
type II Activin/BMP receptors via its finger 2 tip loop. Elife 9, e54582 https://doi.org/10.7554/eLife.54582

90 Lawera, A., Tong, Z., Thorikay, M., Redgrave, R.E., Cai, J., van Dinther, M. et al. (2019) Role of soluble endoglin in BMP9 signaling. Proc. Natl Acad.
Sci. U.S.A. 116, 17800–17808 https://doi.org/10.1073/pnas.1816661116

© 2024 The Author(s). This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY).1528

Biochemical Society Transactions (2024) 52 1515–1528
https://doi.org/10.1042/BST20231547

https://doi.org/10.7554/eLife.54582
https://doi.org/10.1073/pnas.1816661116
https://creativecommons.org/licenses/by/4.0/

	Bone morphogenetic protein signalling in pulmonary arterial hypertension: revisiting the BMPRII connection
	Abstract
	Pulmonary arterial hypertension and bone morphogenetic protein signalling
	Introduction to BMP signalling
	Dysregulated endothelial BMP signalling in the pathogenesis of PAH
	Crystal structures of the BMPRII signalling complex reveal the highly dynamic interaction between BMP10 and BMPRII
	BMPR2 mutations also cause dysregulated BMP signalling in pulmonary smooth muscle cells
	Altered inflammatory response exacerbates loss of BMPRII function and contributes to PAH pathogenesis
	Therapeutic strategies targeting BMP signalling in PAH
	Targeting BMP9 signalling in PAH and controversies over BMP9 signalling
	Sotatercept and ActRIIA-mediated signalling
	Summary and future directions
	Competing Interests
	Funding
	Open Access
	Author Contribution
	References