The combined action of CTCF and its testis-specific paralog BORIS is essential for spermatogenesis

Author:

Rivero-Hinojosa SamuelORCID,Pugacheva Elena M.ORCID,Kang Sungyun,Méndez-Catalá Claudia Fabiola,Kovalchuk Alexander L.ORCID,Strunnikov Alexander V.,Loukinov Dmitri,Lee Jeannie T.ORCID,Lobanenkov Victor V.ORCID

Abstract

AbstractCTCF is a key organizer of the 3D genome. Its specialized paralog, BORIS, heterodimerizes with CTCF but is expressed only in male germ cells and in cancer states. Unexpectedly, BORIS-null mice have only minimal germ cell defects. To understand the CTCF-BORIS relationship, mouse models with varied CTCF and BORIS levels were generated. Whereas Ctcf+/+Boris+/+, Ctcf+/−Boris+/+, and Ctcf+/+Boris−/− males are fertile, Ctcf+/−Boris−/− (Compound Mutant; CM) males are sterile. Testes with combined depletion of both CTCF and BORIS show reduced size, defective meiotic recombination, increased apoptosis, and malformed spermatozoa. Although CM germ cells exhibit only 25% of CTCF WT expression, chromatin binding of CTCF is preferentially lost from CTCF-BORIS heterodimeric sites. Furthermore, CM testes lose the expression of a large number of spermatogenesis genes and gain the expression of developmentally inappropriate genes that are “toxic” to fertility. Thus, a combined action of CTCF and BORIS is required to both repress pre-meiotic genes and activate post-meiotic genes for a complete spermatogenesis program.

Funder

Division of Intramural Research, National Institute of Allergy and Infectious Diseases

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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