Cell Death and Disease (Nov 2024)

MLKL deficiency elevates testosterone production in male mice independently of necroptotic functions

  • Shene Chiou,
  • Wayne Cawthorne,
  • Thomas Soerianto,
  • Vinzenz Hofferek,
  • Komal M. Patel,
  • Sarah E. Garnish,
  • Emma C. Tovey Crutchfield,
  • Cathrine Hall,
  • Joanne M. Hildebrand,
  • Malcolm J. McConville,
  • Kate E. Lawlor,
  • Edwin D. Hawkins,
  • Andre L. Samson,
  • James M. Murphy

DOI
https://doi.org/10.1038/s41419-024-07242-z
Journal volume & issue
Vol. 15, no. 11
pp. 1 – 10

Abstract

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Abstract Mixed lineage kinase domain-like (MLKL) is a pseudokinase, best known for its role as the terminal effector of the necroptotic cell death pathway. MLKL-mediated necroptosis has long been linked to various age-related pathologies including neurodegeneration, atherosclerosis and male reproductive decline, however many of these attributions remain controversial. Here, we investigated the role of MLKL and necroptosis in the adult mouse testis: an organ divided into sperm-producing seminiferous tubules and the surrounding testosterone-producing interstitium. We find that sperm-producing cells within seminiferous tubules lack expression of key necroptotic mediators and thus are resistant to a pro-necroptotic challenge. By comparison, coordinated expression of the necroptotic pathway occurs in the testicular interstitium, rendering cells within this compartment, especially the lysozyme-positive macrophages, vulnerable to necroptotic cell death. We also uncover a non-necroptotic role for MLKL in regulating testosterone levels. Thus, MLKL serves two roles in the mouse testes – one involving the canonical response of macrophages to necroptotic insult, and the other a non-canonical function in male reproductive hormone control.