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1 May 2004 Mitochondria-Dependent Pathway Is Involved in Heat-Induced Male Germ Cell Death: Lessons from Mutant Mice
Yanira Vera, Maruja Diaz-Romero, Susana Rodriguez, Yanhe Lue, Christina Wang, Ronald S. Swerdloff, Amiya P. Sinha Hikim
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Abstract

The signaling events leading to apoptosis can be divided into two major pathways, involving either mitochondria (intrinsic) or death receptors (extrinsic). In a recent study, we have shown the involvement of the mitochondria-dependent apoptotic pathway in heat-induced male germ cell apoptosis in the rat. In additional studies, using the gld (generalized lymphoproliferation disease) and lprcg (lymphoproliferation complementing gld) mice, which harbor loss-of-function mutations in Fas L and Fas, respectively, we have shown that heat-induced germ cell apoptosis is not blocked, thus providing evidence that the Fas signaling system is not required for heat-induced germ cell apoptosis in the testis. In the present study, we have found that the initiation of apoptosis in wild-type mice was preceded by a redistribution of Bax from a cytoplasmic to paranuclear localization in heat-susceptible germ cells. The relocation of Bax is accompanied by sequestration of ultracondensed mitochondria into paranuclear areas of apoptotic germ cells, cytosolic translocation of mitochondrial cytochrome c and DIABLO, and is associated with activation of the initiator caspase 9 and the executioner caspase 3. Similar events were also noted in both gld and lprcg mice. Taken together, these results indicate that the mitochondria-dependent pathway is the key apoptotic pathway for heat-induced male germ cell death in mice.

Yanira Vera, Maruja Diaz-Romero, Susana Rodriguez, Yanhe Lue, Christina Wang, Ronald S. Swerdloff, and Amiya P. Sinha Hikim "Mitochondria-Dependent Pathway Is Involved in Heat-Induced Male Germ Cell Death: Lessons from Mutant Mice," Biology of Reproduction 70(5), 1534-1540, (1 May 2004). https://doi.org/10.1095/biolreprod.103.024661
Received: 24 October 2003; Accepted: 1 January 2004; Published: 1 May 2004
KEYWORDS
Apoptosis
male reproductive tract
spermatogenesis
testis
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