Literature DB >> 30733280

The intramembrane protease SPPL2c promotes male germ cell development by cleaving phospholamban.

Johannes Niemeyer1, Torben Mentrup1,2, Ronny Heidasch3, Stephan A Müller4,5, Uddipta Biswas2, Rieke Meyer1, Alkmini A Papadopoulou6, Verena Dederer3, Martina Haug-Kröper6, Vivian Adamski1, Renate Lüllmann-Rauch7, Martin Bergmann8, Artur Mayerhofer9, Paul Saftig1, Gunther Wennemuth10, Rolf Jessberger2, Regina Fluhrer4,6, Stefan F Lichtenthaler4,5,11, Marius K Lemberg3, Bernd Schröder12,2.   

Abstract

Signal peptide peptidase (SPP) and the four homologous SPP-like (SPPL) proteases constitute a family of intramembrane aspartyl proteases with selectivity for type II-oriented transmembrane segments. Here, we analyse the physiological function of the orphan protease SPPL2c, previously considered to represent a non-expressed pseudogene. We demonstrate proteolytic activity of SPPL2c towards selected tail-anchored proteins. Despite shared ER localisation, SPPL2c and SPP exhibit distinct, though partially overlapping substrate spectra and inhibitory profiles, and are organised in different high molecular weight complexes. Interestingly, SPPL2c is specifically expressed in murine and human testis where it is primarily localised in spermatids. In mice, SPPL2c deficiency leads to a partial loss of elongated spermatids and reduced motility of mature spermatozoa, but preserved fertility. However, matings of male and female SPPL2c -/- mice exhibit reduced litter sizes. Using proteomics we identify the sarco/endoplasmic reticulum Ca2+-ATPase (SERCA2)-regulating protein phospholamban (PLN) as a physiological SPPL2c substrate. Accumulation of PLN correlates with a decrease in intracellular Ca2+ levels in elongated spermatids that likely contribute to the compromised male germ cell differentiation and function of SPPL2c -/- mice.
© 2019 The Authors.

Entities:  

Keywords:  intramembrane proteolysis; phospholamban; signal peptide peptidase‐like proteases; spermatogenesis; tail‐anchored proteins

Mesh:

Substances:

Year:  2019        PMID: 30733280      PMCID: PMC6399600          DOI: 10.15252/embr.201846449

Source DB:  PubMed          Journal:  EMBO Rep        ISSN: 1469-221X            Impact factor:   8.807


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