VCP promotes tTAF-target gene expression and spermatocyte differentiation by downregulating mono-ubiquitylated H2A

Author:

Butsch Tyler J.1ORCID,Dubuisson Olga1,Johnson Alyssa E.1ORCID,Bohnert K. Adam1ORCID

Affiliation:

1. Louisiana State University Department of Biological Sciences , , 202 Life Sciences Building, Baton Rouge, LA 70803 , USA

Abstract

ABSTRACT Valosin-containing protein (VCP) binds and extracts ubiquitylated cargo to regulate protein homeostasis. VCP has been studied primarily in aging and disease contexts, but it also affects germline development. However, the precise molecular functions of VCP in the germline, particularly in males, are poorly understood. Using the Drosophila male germline as a model system, we find that VCP translocates from the cytosol to the nucleus as germ cells transition into the meiotic spermatocyte stage. Importantly, nuclear translocation of VCP appears to be one crucial event stimulated by testis-specific TBP-associated factors (tTAFs) to drive spermatocyte differentiation. VCP promotes the expression of several tTAF-target genes, and VCP knockdown, like tTAF loss of function, causes cells to arrest in early meiotic stages. At a molecular level, VCP activity supports spermatocyte gene expression by downregulating a repressive histone modification, mono-ubiquitylated H2A (H2Aub), during meiosis. Remarkably, experimentally blocking H2Aub in VCP-RNAi testes is sufficient to overcome the meiotic-arrest phenotype and to promote development through the spermatocyte stage. Collectively, our data highlight VCP as a downstream effector of tTAFs that downregulates H2Aub to facilitate meiotic progression.

Funder

Office of Research and Economic Development, Louisiana State University

LSU College of Science

National Institutes of Health

National Institute of General Medical Sciences

Louisiana State University

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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