Cyp26 enzymes are required to balance the cardiac and vascular lineages within the anterior lateral plate mesoderm

Rydeen, Ariel B.; Waxman, Joshua S.

doi:10.1242/dev.105874

Cited by 35 publications

(64 citation statements)

References 50 publications

(103 reference statements)

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“…Increases in RA signaling can inhibit cardiomyocyte specification, while decreases in RA signaling can promote cardiomyocyte specification (Keegan et al, 2005; Rydeen and Waxman, 2014; Waxman and Yelon, 2009). Interestingly, examining heart morphology, cell number, and cardiomyocyte marker expression, we found that the hearts of vp-rar mRNA-injected Tg(-5.1myl7:DsRed-NLS) f2 embryos (Mably et al, 2003) were enlarged, had increased cell number, and increased cardiomyocyte marker expression at 48 hpf (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…6B-B3, D-D3, E), which suggests the vp-rar expression can promote cell non-autonomous loss of RA signaling. Next, to determine if the cell non-autonomous effects of vp-rar expression were dependent on Cyp26a1, we transplanted RA sensor donor cells into WT hosts or hosts co-injected with vp-rar mRNA and previously characterized cyp26a1 MOs (D’Aniello et al, 2013; Rydeen and Waxman, 2014). In contrast to when RA sensor cells were transplanted into vp-rar mRNA injected hosts, we found that depletion of Cyp26a1 in vp-rar mRNA injected host embryos results in RA sensor donor cells with robust GFP expression (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Cyp26a1 mRNA was injected at 500pg as previously described (Kudoh et al, 2002). Previously published cyp26a1 MOs were injected using a cocktail of 2–4ng cyp26a1 MO1 and 1–2ng cyp26a1 MO2, as well as 3ng p53 MO to combat non-specific cell death (D’Aniello et al, 2013; Rydeen and Waxman, 2014). …”

Section: Methodsmentioning

confidence: 99%

“…RT-qPCR was performed as has been previously described (D’Aniello et al, 2013; Rydeen and Waxman, 2014). Whole embryo RNA was obtained from pooled groups of 30 embryos, which were homogenized in Trizol (Ambion) and isolated using Purelink RNA Microkit (Invitrogen).…”

Section: Methodsmentioning

confidence: 99%

“…Similarly, in zebrafish, Martin and Kimelman (2010) found that Cyp26a1 does not have cell autonomous roles within mesodermal progenitor pool, suggesting non-autonomous functions. Furthermore, recent work from our lab has suggested that loss of Cyp26 enzymes can have cell non-autonomous consequences in patterning the cardiovascular progenitor fields within the anterior lateral plate mesoderm (Rydeen and Waxman, 2014). Additionally, using computational modeling, White et al (2007) proposed a model in zebrafish embryos where the embryonic RA gradient is shaped through self-enhanced degradation by promoting Cyp26a1 expression, in effect arguing that Cyp26a1 may have cell autonomous and cell non-autonomous consequences in shaping the embryonic RA gradient.…”

Section: Introductionmentioning

confidence: 99%

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Excessive feedback of Cyp26a1 promotes cell non-autonomous loss of retinoic acid signaling

Rydeen

Voisin

D’Aniello

et al. 2015

Developmental Biology

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Teratogenic levels of retinoic acid (RA) signaling can cause seemingly contradictory phenotypes indicative of both increases and decreases of RA signaling. However, the mechanisms underlying these contradictory phenotypes are not completely understood. Here, we report that using a hyperactive RA receptor to enhance RA signaling in zebrafish embryos leads to defects associated with gain and loss of RA signaling. While the gain-of-function phenotypes arise from an initial increase in RA signaling, using genetic epistasis analysis we found that the loss-of-function phenotypes result from a clearing of embryonic RA that requires a rapid and dramatic increase in cyp26a1 expression. Thus, the sensitivity of cyp26a1 expression to increased RA signaling causes an overcompensation of negative feedback and loss of embryonic RA signaling. Additionally, we used blastula transplantation experiments to test if Cyp26a1, despite its cellular localization, can limit RA exposure to neighboring cells. We find that enhanced Cyp26a1 expression limits RA signaling in the local environment, thus providing the first direct evidence that Cyp26 enzymes can have cell non-autonomous consequences on RA levels within tissues. Therefore, our results provide novel insights into the teratogenic mechanisms of RA signaling and the cellular mechanisms by which Cyp26a1 expression can shape a RA gradient.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Excessive feedback of Cyp26a1 promotes cell non-autonomous loss of retinoic acid signaling

Rydeen

Voisin

D’Aniello

et al. 2015

Developmental Biology

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Input overload: Contributions of retinoic acid signaling feedback mechanisms to heart development and teratogenesis

D’Aniello

Waxman

2015

Developmental Dynamics

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Appropriate levels of retinoic acid (RA) signaling are critical for normal heart development in vertebrates. A fascinating property of RA signaling is the thoroughness by which positive and negative feedback are employed to promote proper embryonic RA levels. In the present short review, we first cover the advancement of hypotheses regarding the impact of RA signaling on cardiac specification. We then discuss our current understanding of RA signaling feedback mechanisms and the implications of recent studies, which have indicated improperly maintained RA signaling feedback can be a contributing factor to developmental malformations. Developmental Dynamics 244:513–523, 2015. © 2014 Wiley Periodicals, Inc.

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Retinoic acid signaling in heart development

Nakajima

2019

Genesis

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Summary Retinoic acid (RA) is a vitamin A metabolite that acts as a morphogen and teratogen. Excess or defective RA signaling causes developmental defects including in the heart. The heart develops from the anterior lateral plate mesoderm. Cardiogenesis involves successive steps, including formation of the primitive heart tube, cardiac looping, septation, chamber development, coronary vascularization, and completion of the four‐chambered heart. RA is dispensable for primitive heart tube formation. Before looping, RA is required to define the anterior/posterior boundaries of the heart‐forming mesoderm as well as to form the atrium and sinus venosus. In outflow tract elongation and septation, RA signaling is required to maintain/differentiate cardiogenic progenitors in the second heart field at the posterior pharyngeal arches level. Epicardium‐secreted insulin‐like growth factor, the expression of which is regulated by hepatic mesoderm‐derived erythropoietin under the control of RA, promotes myocardial proliferation of the ventricular wall. Epicardium‐derived RA induces the expression of angiogenic factors in the myocardium to form the coronary vasculature. In cardiogenic events at different stages, properly controlled RA signaling is required to establish the functional heart.

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Cyp26 enzymes are required to balance the cardiac and vascular lineages within the anterior lateral plate mesoderm

Cited by 35 publications

References 50 publications

Excessive feedback of Cyp26a1 promotes cell non-autonomous loss of retinoic acid signaling

Excessive feedback of Cyp26a1 promotes cell non-autonomous loss of retinoic acid signaling

Input overload: Contributions of retinoic acid signaling feedback mechanisms to heart development and teratogenesis

Retinoic acid signaling in heart development

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