Abstract

Craniofacial defects, such as cleft lip and/or palate, are the most prevalent congenital malformations worldwide. The cranial neural crest, an essential contributor to the facial skeleton, requires platelet derived growth factor (PDGF) signaling. In humans, SNPs in the PDGFC regulatory region are associated with cleft lip and palate. In mice, loss of PDGF Receptor (PDGFR) or its ligands, PDGFA and PDGFC, results in facial clefting. Previous work has shown that PDGFR is required cell autonomously in the neural crest for craniofacial development. My project focuses on determining novel transcriptional pathways downstream of PDGFR critical for craniofacial development. We adopted a next generation sequencing approach using mouse embryonic palatal mesenchyme (MEPM) cells to identify PDGF responsive genes on a genome wide scale in a physiologically relevant system. To this end, we stimulated primary mouse embryonic palatal mesenchyme (MEPM) cells with PDGFA and performed RNA-seq at 0, 1, and 4 hours. Analysis of this dataset yielded seven candidate transcriptional pathways regulated by PDGF signaling. To limit the scope of our studies for this proposal, we focus on Serum Response Factor (SRF), an important transcriptional regulator of actin dynamics that we found compelling given the classic function of PDGF in modulating the actin cytoskeleton. Mice harboring conditional deletion of SRF in the neural crest display both cardiac and craniofacial defects; excitingly, further investigation uncovered a previously unreported overt facial cleft in these mice. In addition, many transcriptional targets of SRF (ActB, FlnA, and MyH9) are implicated in human craniofacial development. By studying the interactions between PDGF signaling and SRF activity, we will build the foundation required to design innovative diagnostic and therapeutic strategies targeting these fundamental pathways.

Public Health Relevance

Craniofacial defects, such as cleft lip and/or palate, are the most prevalent congenital malformations worldwide. The focus of this proposal is to study the transcriptional targets activated by PDGF signaling during craniofacial development. Our results will lead to a better understanding of the pathways underlying development of the midface.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Predoctoral Individual National Research Service Award (F31)
Project #
5F31DE023456-03
Application #
8824509
Study Section
NIDR Special Grants Review Committee (DSR)
Program Officer
Frieden, Leslie A
Project Start
2013-05-01
Project End
2015-06-30
Budget Start
2015-05-01
Budget End
2015-06-30
Support Year
3
Fiscal Year
2015
Total Cost
Indirect Cost

  Institution

Name
Icahn School of Medicine at Mount Sinai
Department
Biology
Type
Schools of Medicine
DUNS #
078861598
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Vasudevan, Harish N; Soriano, Philippe (2016) A Thousand and One Receptor Tyrosine Kinases: Wherein the Specificity? Curr Top Dev Biol 117:393-404
Vasudevan, Harish N; Mazot, Pierre; He, Fenglei et al. (2015) Receptor tyrosine kinases modulate distinct transcriptional programs by differential usage of intracellular pathways. Elife 4:
Vasudevan, Harish N; Soriano, Philippe (2014) SRF regulates craniofacial development through selective recruitment of MRTF cofactors by PDGF signaling. Dev Cell 31:332-344