Identification of ancestral gnathostome Gli3 enhancers with activity in mammals

Author:

Ali Shahid12,Abrar Muhammad1,Hussain Irfan1,Batool Fatima1,Raza Rabail Zehra3,Khatoon Hizran1,Zoia Matteo4,Visel Axel567,Shubin Neil H.2,Osterwalder Marco48,Abbasi Amir Ali1ORCID

Affiliation:

1. National Center for Bioinformatics, Program of Comparative and Evolutionary Genomics, Faculty of Biological Sciences, Quaid‐i‐Azam University Islamabad Pakistan

2. Department of Organismal Biology and Anatomy The University of Chicago Chicago Illinois USA

3. Department of Biological Sciences Faculty of Multidisciplinary Studies, National University of Medical Sciences Rawalpindi Pakistan

4. Department for Biomedical Research (DBMR) University of Bern Bern Switzerland

5. Environmental Genomics and System Biology Division Lawrence Berkeley National Laboratory Berkeley California USA

6. U.S. Department of Energy Joint Genome Institute Berkeley California USA

7. School of Natural Sciences, University of California, Merced Merced California USA

8. Department of Cardiology, Bern University Hospital Bern Switzerland

Abstract

AbstractAbnormal expression of the transcriptional regulator and hedgehog (Hh) signaling pathway effector Gli3 is known to trigger congenital disease, most frequently affecting the central nervous system (CNS) and the limbs. Accurate delineation of the genomic cis‐regulatory landscape controlling Gli3 transcription during embryonic development is critical for the interpretation of noncoding variants associated with congenital defects. Here, we employed a comparative genomic analysis on fish species with a slow rate of molecular evolution to identify seven previously unknown conserved noncoding elements (CNEs) in Gli3 intronic intervals (CNE15–21). Transgenic assays in zebrafish revealed that most of these elements drive activities in Gli3 expressing tissues, predominantly the fins, CNS, and the heart. Intersection of these CNEs with human disease associated SNPs identified CNE15 as a putative mammalian craniofacial enhancer, with conserved activity in vertebrates and potentially affected by mutation associated with human craniofacial morphology. Finally, comparative functional dissection of an appendage‐specific CNE conserved in slowly evolving fish (elephant shark), but not in teleost (CNE14/hs1586) indicates co‐option of limb specificity from other tissues prior to the divergence of amniotes and lobe‐finned fish. These results uncover a novel subset of intronic Gli3 enhancers that arose in the common ancestor of gnathostomes and whose sequence components were likely gradually modified in other species during the process of evolutionary diversification.

Funder

Higher Education Commision, Pakistan

Schweizerischer Nationalfonds zur Förderung der Wissenschaftlichen Forschung

Publisher

Wiley

Subject

Cell Biology,Developmental Biology

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