PRDM16 co-operates with LHX2 to shape the human brain

Author:

Suresh Varun123,Bhattacharya Bidisha12,Tshuva Rami Yair12,Danan Gotthold Miri12,Olender Tsviya12,Bose Mahima3,Pradhan Saurabh J45,Zeev Bruria Ben6,Smith Richard Scott7,Tole Shubha3,Galande Sanjeev48,Harwell Corey C91011,Baizabal José-Manuel12,Reiner Orly12

Affiliation:

1. Weizmann Institute of Science Department of Molecular Genetics, , 234 Herzl St., Rehovot 7610001, Israel

2. Weizmann Institute of Science Department of Molecular Neuroscience, , 234 Herzl St., Rehovot 7610001, Israel

3. Tata Institute of Fundamental Research Department of Biological Sciences, , Homi Bhabha Road, Navy Nagar, Colaba, Mumbai 400005, India

4. Indian Institute of Science Education and Research Pune Chromatin Biology and Epigenetics Laboratory, Biology Department, , Dr. Homi Bhabha Road, Pune 411008, India

5. Institute of Molecular Biotechnology of the Austrian Academy of Sciences, Vienna Biocenter , 3 Dr. Bohr-Gasse, 1030 Vienna, Austria

6. Tel Aviv University Edmond and Lily Safra Pediatric Hospital, Sheba Medical Center and Tel Aviv School of Medicine, , Ramat Aviv 69978, Israel

7. Northwestern University Feinberg School of Medicine Department of Pharmacology, , 320 E. Superior St., Chicago, IL 60611, USA

8. Center of Excellence in Epigenetics, Shiv Nadar University Department of Life Sciences, , Shiv Nadar IoE, Gautam Buddha Nagar, Uttar Pradesh - 201314, India

9. University of California, San Francisco Eli and Edythe Broad Center of Regeneration Medicine and Stem Cell Research, , 35 Medical Center Way, San Francisco, CA 94143, USA

10. Weill Institute for Neuroscience , 1651 4th St, San Francisco, CA94158, USA

11. University of California, San Francisco Department of Neurology, , 505 Parnassus Ave, San Francisco, CA 94143, USA

12. Indiana University Department of Biology, , 1001 E 3rd St., Bloomington, IN 47405, USA

Abstract

Abstract PRDM16 is a dynamic transcriptional regulator of various stem cell niches, including adipocytic, hematopoietic, cardiac progenitors, and neural stem cells. PRDM16 has been suggested to contribute to 1p36 deletion syndrome, one of the most prevalent subtelomeric microdeletion syndromes. We report a patient with a de novo nonsense mutation in the PRDM16 coding sequence, accompanied by lissencephaly and microcephaly features. Human stem cells were genetically modified to mimic this mutation, generating cortical organoids that exhibited altered cell cycle dynamics. RNA sequencing of cortical organoids at day 32 unveiled changes in cell adhesion and WNT-signaling pathways. ChIP-seq of PRDM16 identified binding sites in postmortem human fetal cortex, indicating the conservation of PRDM16 binding to developmental genes in mice and humans, potentially at enhancer sites. A shared motif between PRDM16 and LHX2 was identified and further examined through comparison with LHX2 ChIP-seq data from mice. These results suggested a collaborative partnership between PRDM16 and LHX2 in regulating a common set of genes and pathways in cortical radial glia cells, possibly via their synergistic involvement in cortical development.

Funder

Department of Science and Technology, Govt. of India

Tata Institute of Fundamental Research

Canadian Institutes of Health Research

Science and Engineering Research Board, Government of India

Centre of Excellence in Epigenetics program of the Department of Biotechnology Government of India

Weizmann Institute of Science

National Institute Of Neurological Disorders And Stroke of the National Institutes of Health

United States-Israel Binational Science Foundation

Weizmann SABRA—Yeda-Sela—WRC Program

Publisher

Oxford University Press (OUP)

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