Lmx1b-targeted cis-regulatory modules involved in limb dorsalization

Author:

Haro Endika1,Watson Billy A.1,Feenstra Jennifer M.1,Tegeler Luke1,Pira Charmaine U.1,Mohan Subburaman2,Oberg Kerby C.1ORCID

Affiliation:

1. Department of Pathology and Human Anatomy, Loma Linda University, Loma Linda, CA, USA

2. Musculoskeletal Disease Center, Loma Linda VA HealthCare System, Loma Linda, CA, USA

Abstract

Lmx1b is a homeodomain transcription factor responsible for limb dorsalization. Despite striking double-ventral (loss-of-function) and double-dorsal (gain-of-function) limb phenotypes, no direct gene targets in the limb have been confirmed. To determine direct targets, we performed a chromatin immunoprecipitation against Lmx1b at E12.5 followed by next generation sequencing (ChIP-seq). Nearly 84% (n=617) of the Lmx1b-bound genomic intervals (LBIs) identified overlap with chromatin regulatory marks indicative of potential cis-regulatory modules (PCRMs). In addition, 73 LBIs mapped to known CRMs active during limb development. We compared Lmx1b-bound PCRMs to genes differentially expressed by Lmx1b and found 292 PCRMs within 1 Mb of 254 Lmx1b-regulated genes. Gene ontologic analysis suggests that Lmx1b targets extracellular matrix production, bone/joint formation, axonal guidance, vascular development, cell proliferation and cell movement. We validated the functional activity of a PCRM associated with joint-related Gdf5 that provides a mechanism for Lmx1b-mediated joint modification and a PCRM associated with Lmx1b that suggests a role in autoregulation. This is the first report to describe genome-wide Lmx1b binding during limb development, directly linking Lmx1b to targets that accomplish limb dorsalization.

Funder

National Organization for Rare Disorders

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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