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30 September 2023 Targeted mutation and inactivation of the kinesin light chain 3 protein-encoding gene have no impact on mouse fertility
Nathalie Daniel-Carlier, Johan Castille, Bruno Passet, Marthe Vilotte, Christelle Le Danvic, Florence Jaffrezic, Christian Beauvallet, Christine Péchoux, Aurélien Capitan, Jean-luc Vilotte
Author Affiliations +
Abstract

The kinesin light chain 3 protein (KLC3) is the only member of the kinesin light chain protein family that was identified in post-meiotic mouse male germ cells. It plays a role in the formation of the sperm midpiece through its association with both spermatid mitochondria and outer dense fibers (ODF). Previous studies showed a significant correlation between its expression level and sperm motility and quantitative semen parameters in humans, while the overexpression of a KLC3-mutant protein unable to bind ODF also affected the same traits in mice. To further assess the role of KLC3 in fertility, we used CRISPR/Cas9 genome editing in mice and investigated the phenotypes induced by the invalidation of the gene or of a functional domain of the protein. Both approaches gave similar results, i.e. no detectable change in male or female fertility. Testis histology, litter size and sperm count were not altered. Apart from the line-dependent alterations of Klc3 mRNA levels, testicular transcriptome analysis did not reveal any other changes in the genes tested. Western analysis supported the absence of KLC3 in the gonads of males homozygous for the inactivating mutation and a strong decrease in expression in males homozygous for the allele lacking one out of the five tetratricopeptide repeats. Overall, these observations raise questions about the supposedly critical role of this kinesin in reproduction, at least in mice where its gene mutation or inactivation did not translate into fertility impairment.

Summary Sentence

Although the kinesin light chain 3 protein has been proposed to play a critical role in midpiece formation and sperm parameters in humans and mice, mutation or inactivation of its encoding gene has no adverse effect on mouse fertility.

Graphical Abstract

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Nathalie Daniel-Carlier, Johan Castille, Bruno Passet, Marthe Vilotte, Christelle Le Danvic, Florence Jaffrezic, Christian Beauvallet, Christine Péchoux, Aurélien Capitan, and Jean-luc Vilotte "Targeted mutation and inactivation of the kinesin light chain 3 protein-encoding gene have no impact on mouse fertility," Biology of Reproduction 110(1), 75-86, (30 September 2023). https://doi.org/10.1093/biolre/ioad131
Published: 30 September 2023
KEYWORDS
CRISPR
fertility
genome editing
human
Klc3
Mouse
sperm
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