A myocardial lineage derives from Tbx18 epicardial cells

Cai, Chen-Leng; Martin, Jody; Sun, Yunfu; Cui, Li; Wang, Lianchun; Ouyang, Kunfu; Yang, Lei; Bu, Lei; Liang, Xingqun; Zhang, Xiaoxue; Stallcup, William B.; Denton, Christopher P.; McCulloch, Andrew D.; Chen, Ju; Evans, Sylvia M.

doi:10.1038/nature06969

Cited by 712 publications

(772 citation statements)

References 28 publications

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“…Using this strategy, we have created a RA-responsive Cre line, and shown through crosses with the R26R reporter strain that, at early embryonic stages, it results in a pattern of activity virtually identical to that of the lacZ transgene originally created by Rossant et al (1991), and driven by the same RARE-hsp68 composite promoter. As observed for other Cre;R26R studies (e.g., Jiang et al, 2000;Zhang et al, 2003;Huynh et al, 2007;Cai et al, 2008), lacZ activity is stably inherited in RARE-Cre;R26R double transgenic mice, allowing a lineage tracing of the Cre-excised cells. The RARE-Cre transgene described herein will thus be a useful tool for any future work aiming to map the distribution of retinoid-sensitive cell lineages in specific developing systems.…”

Section: Discussionsupporting

confidence: 57%

“…This correlates with ''late'' effects of RA in regulating myocardial compact zone growth by inducing growth factor signaling and/or cardiomyocyte differentiation (Merki et al, 2005;Lin et al, 2010), and potentially in regulating the epicardial to myocardial lineage conversion (Cai et al, 2008;Zhou et al, 2008). It is noteworthy that a large part of the myocardium (i.e.…”

Section: Discussionmentioning

confidence: 75%

“…As in other murine lineage studies (e.g., Jiang et al, 2000;Zhang et al, 2003;Huynh et al, 2007;Cai et al, 2008), our strategy uses an ''effector'' transgene driving expression of the Cre recombinase upon RA activation, and a reporter line (the R26R reporter) expressing a functional lacZ gene after Cre-dependent excision of a STOP sequence (Soriano, 1999). We generated transgenic mice in which Cre is driven by the same RARE-hsp68 sequence as in the ''parental'' RARE-hsp68-lacZ transgene (Rossant et al, 1991), and crossed these with R26R reporter mice.…”

Section: Introductionmentioning

confidence: 68%

“…These include (i) the ''first heart field'' or cardiac crescent formed from mesoderm emerging from the primitive streak (Garcia-Martinez and Schoenwolf, 1993;Tam et al, 1997); (ii) the ''second heart field'' originating from pharyngeal mesoderm (Buckingham et al, 2005); (iii) the (pro)epicardium, a population originating and giving rise to coronary vasculature, myocardial fibroblasts and to a distinct cardiomyocytic lineage (Cai et al, 2008;Zhou et al, 2008), and (iv) the ''cardiac'' neural crest, a subset of post-otic neural crest cells migrating through the third to sixth branchial arches and participating to the development of the aortic arches and aorticopulmonary septum (reviewed by Rochais et al, 2009). All these lineages have been reported to be influenced by embryonic RA (Hochgreb et al, 2003;Ryckebusch et al, 2008;Sirbu et al, 2008;Dupe and Pellerin, 2009), although recent studies implicate the second heart field (Ryckebusch et al, 2008;Sirbu et al, 2008) and the epicardium (Merki et al, 2005;Lin et al, 2010) as the main sites of RA signaling.…”

Section: Branchial Arches and Heartmentioning

confidence: 99%

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Fate of retinoic acid–activated embryonic cell lineages

Dollé

Fraulob

Gallego-Llamas

et al. 2010

Developmental Dynamics

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Retinoic acid (RA), a vitamin A derivative, is synthesized by specific cell populations and acts as a diffusible embryonic signal activating ligand‐inducible transcription factors, the RA receptors (RARs). RA‐activatable transgenic systems have revealed many discrete, transient sites of RA action during development. However, there has been no attempt to permanently label the RA‐activated cell lineages during mouse ontogenesis. We describe the characterization of a RA‐activatable Cre transgene, which through crosses with a conditional reporter strain (the ROSA26R lacZ reporter), leads to a stable labeling of the cell populations experiencing RA signaling during embryogenesis. RA response‐element (RARE) ‐driven Cre activity mimics at early stages the known activity of the corresponding RARE‐lacZ transgene (Rossant et al.,1991). Stable labeling of the Cre‐excised cell populations allows to trace the distribution of the RA‐activated cell lineages at later stages. These are described in relationship with current models of RA activity in various developmental systems, including the embryonic caudal region, limb buds, hindbrain, sensory organs, and heart. Developmental Dynamics 239:3260–3274, 2010. © 2010 Wiley‐Liss, Inc.

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Section: Discussionsupporting

confidence: 57%

Section: Discussionmentioning

confidence: 75%

Section: Introductionmentioning

confidence: 68%

Section: Branchial Arches and Heartmentioning

confidence: 99%

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Fate of retinoic acid–activated embryonic cell lineages

Dollé

Fraulob

Gallego-Llamas

et al. 2010

Developmental Dynamics

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“…The mainstream view of coronary artery formation from PE-derived ECs has been re-evaluated over the past decade through the use of Cre-LoxP genetic lineage-tracing approaches in mice [4][5][6][7]. Several different mouse Cre lines that label populations within the PE were developed.…”

mentioning

confidence: 99%

The mysterious origins of coronary vessels

Zhang

2013

Cell Res

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Fibroblast‐mediated intercellular crosstalk in the healthy and diseased heart

et al. 2021

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Cardiac fibroblasts constitute a major cell population in the heart. They secrete extracellular matrix components and various other factors shaping the microenvironment of the heart. In silico analysis of intercellular communication based on single‐cell RNA sequencing revealed that fibroblasts are the source of the majority of outgoing signals to other cell types. This observation suggests that fibroblasts play key roles in orchestrating cellular interactions that maintain organ homeostasis but that can also contribute to disease states. Here, we will review the current knowledge of fibroblast interactions in the healthy, diseased, and aging heart. We focus on the interactions that fibroblasts establish with other cells of the heart, specifically cardiomyocytes, endothelial cells and immune cells, and particularly those relying on paracrine, electrical, and exosomal communication modes.

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A myocardial lineage derives from Tbx18 epicardial cells

Cited by 712 publications

References 28 publications

Fate of retinoic acid–activated embryonic cell lineages

Fate of retinoic acid–activated embryonic cell lineages

The mysterious origins of coronary vessels

Fibroblast‐mediated intercellular crosstalk in the healthy and diseased heart

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