Interaction between <i>alk1</i> and blood flow in the development of arteriovenous malformations

Cortí, Paola; Young, Sarah P.; Chen, Chia Yuan; Patrick, Michael J.; Rochon, Elizabeth R.; Pekkan, Kerem; Roman, Beth L.

doi:10.1242/dev.060467

Cited by 191 publications

(269 citation statements)

References 56 publications

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“…Both of these genes are flow responsive in cultured endothelial cells (Wang et al, 1993;Melchionna et al, 2005), suggesting that Alk1 might lie upstream of cxcr4a and edn1 in a mechanosensitive signaling pathway. In support of this hypothesis, blood flowmediated repression of cxcr4a correlates with diminished endothelial cell protrusive activity in nascent zebrafish arteries (Bussmann et al, 2011), and zebrafish alk1 mutants, which exhibit abnormally high levels of arterial cxcr4a, develop enlarged arteries containing supernumerary endothelial cells, suggestive of failed flow-induced suppression of endothelial cell migration or proliferation (Roman et al, 2002;Corti et al, 2011). Evidence from mice further supports the idea that Alk1 functions in a flowresponsive pathway to promote quiescence of nascent arteries.…”

Section: Introductionmentioning

confidence: 90%

“…When appropriate, embryo medium was supplemented with 0.003% phenylthiourea (PTU) (Sigma, St Louis, MO, USA) at 24 hours post-fertilization (hpf) to prevent melanin synthesis. Mutant line alk1 y6 and the alk1 y6 genotyping assay have been described previously (Roman et al, 2002 have been described previously (Roman et al, 2002;Traver et al, 2003;Choi et al, 2007;Corti et al, 2011 (Villefranc et al, 2007), pME-alk1 and p3E-MTpA (Kwan et al, 2007). To drive ligand-and type II receptor-independent, constitutively active alk1 (Roman et al, 2002) in endothelial cells, we generated ptolfli1a.ebs:alk1 CA -mCherry, recombining pDESTtol2pA2, p5E fli1a.ebs (fli1a Ets-binding site; a kind gift from N. Lawson, University of Massachusetts Medical School, Worcester, MA, USA), pME alk1 CA and p3E mCherry-pA (Kwan et al, 2007).…”

Section: Zebrafish Lines and Maintenancementioning

confidence: 99%

“…We could not rescue bmp10 or bmp10-like morphant phenotypes by injecting morpholino-resistant mRNA because embryos ventralized (data not shown). The alk1, tnnt2a and control morpholinos have been described previously (Sehnert et al, 2002;Corti et al, 2011).…”

Section: Zebrafish Lines and Maintenancementioning

confidence: 99%

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Circulating Bmp10 acts through endothelial Alk1 to mediate flow-dependent arterial quiescence

et al. 2013

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SUMMARYBlood flow plays crucial roles in vascular development, remodeling and homeostasis, but the molecular pathways required for transducing flow signals are not well understood. In zebrafish embryos, arterial expression of activin receptor-like kinase 1 (alk1), which encodes a TGFβ family type I receptor, is dependent on blood flow, and loss of alk1 mimics lack of blood flow in terms of dysregulation of a subset of flow-responsive arterial genes and increased arterial endothelial cell number. These data suggest that blood flow activates Alk1 signaling to promote a flow-responsive gene expression program that limits nascent arterial caliber. Here, we demonstrate that restoration of endothelial alk1 expression to flow-deprived arteries fails to rescue Alk1 activity or normalize arterial endothelial cell gene expression or number, implying that blood flow may play an additional role in Alk1 signaling independent of alk1 induction. To this end, we define cardiac-derived Bmp10 as the crucial ligand for endothelial Alk1 in embryonic vascular development, and provide evidence that circulating Bmp10 acts through endothelial Alk1 to limit endothelial cell number in and thereby stabilize the caliber of nascent arteries. Thus, blood flow promotes Alk1 activity by concomitantly inducing alk1 expression and distributing Bmp10, thereby reinforcing this signaling pathway, which functions to limit arterial caliber at the onset of flow. Because mutations in ALK1 cause arteriovenous malformations (AVMs), our findings suggest that an impaired flow response initiates AVM development.

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Section: Introductionmentioning

confidence: 90%

Section: Zebrafish Lines and Maintenancementioning

confidence: 99%

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Circulating Bmp10 acts through endothelial Alk1 to mediate flow-dependent arterial quiescence

et al. 2013

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“…Increased Pai1 suggests increased TGFβ signaling following endothelial deletion of Rbpj. Mutations in TGFβ pathway members are associated with AVMs in humans, mice and zebrafish (Corti et al, 2011;Johnson et al, 1996;Kim et al, 2012;McAllister et al, 1994;Park et al, 2008Park et al, , 2009Urness et al, 2000). Recently, TGFβ and Notch were shown to synergistically regulate retinal vascular morphogenesis (Larrivee et al, 2012) and BAVM formation (Yao et al, 2013) in mice.…”

Section: Loss Of Endothelial Rbpj Alters a Downstream Tgfβ Effector Imentioning

confidence: 99%

Deletion of Rbpj from postnatal endothelium leads to abnormal arteriovenous shunting in mice

et al. 2014

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Arteriovenous malformations (AVMs) are tortuous vessels characterized by arteriovenous (AV) shunts, which displace capillaries and shunt blood directly from artery to vein. Notch signaling regulates embryonic AV specification by promoting arterial, as opposed to venous, endothelial cell (EC) fate. To understand the essential role of endothelial Notch signaling in postnatal AV organization, we used inducible Cre-loxP recombination to delete Rbpj, a mediator of canonical Notch signaling, from postnatal ECs in mice. Deletion of endothelial Rbpj from birth resulted in features of AVMs by P14, including abnormal AV shunting and tortuous vessels in the brain, intestine and heart. We further analyzed brain AVMs, as they pose particular health risks. Consistent with AVM pathology, we found cerebral hemorrhage, hypoxia and necrosis, and neurological deficits. AV shunts originated from capillaries (and possibly venules), with the earliest detectable morphological abnormalities in AV connections by P8. Prior to AV shunt formation, alterations in EC gene expression were detected, including decreased Efnb2 and increased Pai1, which encodes a downstream effector of TGFβ signaling. After AV shunts had formed, whole-mount immunostaining showed decreased Efnb2 and increased Ephb4 expression within AV shunts, suggesting that ECs were reprogrammed from arterial to venous identity. Deletion of Rbpj from adult ECs led to tortuosities in gastrointestinal, uterine and skin vascular beds, but had mild effects in the brain. Our results demonstrate a temporal requirement for Rbpj in postnatal ECs to maintain proper artery, capillary and vein organization and to prevent abnormal AV shunting and AVM pathogenesis.

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“…Though the exact molecular mechanisms involved in the relationship between aortic arch hemodynamics, gene expression, and tissue remodeling are not yet fully understood, τ w is believed to be the primary mechanical stimulus for vascular remodeling (Culver and Dickinson 2010;Rodbard 1975), clinically referred to as the "flow-dependency principle" (Kamiya and Togawa 1980;Lu et al 2001;Rodbard 1975). The temporal and spatial events associated with flow sensitive altered aortic morphogenesis (at the first aortic arch) in the Akl-1 mutant zebrafish model can be more complex as illustrated by recent studies Corti et al 2011;Patrick et al 2011). …”

Section: Introductionmentioning

confidence: 99%

Computational hemodynamic optimization predicts dominant aortic arch selection is driven by embryonic outflow tract orientation in the chick embryo

Kowalski

Teslovich

Dur

et al. 2012

Biomech Model Mechanobiol

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In the early embryo, a series of symmetric, paired vessels, the aortic arches, surround the foregut and distribute cardiac output to the growing embryo and fetus. During embryonic development the arch vessels undergo large-scale asymmetric morphogenesis to form species-specific adult great vessel patterns. These transformations occur within a dynamic biomechanical environment, which can play an important role in the development of normal arch configurations or the aberrant arch morphologies associated with congenital cardiac defects. Arrested migration and rotation of the embryonic outflow tract during late stages of cardiac looping has been shown to produce both outflow tract and several arch abnormalities. Here we investigate how changes in flow distribution

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Interaction between alk1 and blood flow in the development of arteriovenous malformations

Cited by 191 publications

References 56 publications

Circulating Bmp10 acts through endothelial Alk1 to mediate flow-dependent arterial quiescence

Circulating Bmp10 acts through endothelial Alk1 to mediate flow-dependent arterial quiescence

Deletion of Rbpj from postnatal endothelium leads to abnormal arteriovenous shunting in mice

Computational hemodynamic optimization predicts dominant aortic arch selection is driven by embryonic outflow tract orientation in the chick embryo

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