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      Expression of a mitochondrial progesterone receptor in human spermatozoa correlates with a progestin-dependent increase in mitochondrial membrane potential.

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          Abstract

          The hyperactivation of human spermatozoa necessary for fertilization requires a substantial increase in cellular energy production. The factors responsible for increasing cellular energy remain poorly defined. This article proposes a role for a novel mitochondrial progesterone receptor (PR-M) in modulation of mitochondrial activity. Basic science studies demonstrate a 38 kDa protein with western blot analysis, consistent with PR-M; whereas imaging studies with confocal and immunoelectron microscopy demonstrate a PR on the mitochondria. Treatment with a PR-specific progestin shows increased mitochondrial membrane potential, not related to induction of an acrosome reaction. The increase in mitochondrial membrane potential was inhibited by a specific PR antagonist, but not affected by an inhibitor to the progesterone-dependent Catsper voltage-activated channel. In conclusion, these studies suggest expression of a novel mitochondrial PR in human spermatozoa with a progestin-dependent increase in mitochondrial activity. This mechanism may serve to enhance cellular energy production as the spermatozoa traverse the female genital tract being exposed to increasing concentrations of progesterone.

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          Author and article information

          Journal
          Andrology
          Andrology
          Wiley
          2047-2927
          2047-2919
          Nov 2014
          : 2
          : 6
          Affiliations
          [1 ] Department of Obstetrics and Gynecology, Duke University, Durham, NC, USA.
          Article
          NIHMS663405
          10.1111/j.2047-2927.2014.00263.x
          4340691
          25187426
          fff4fecf-08f2-461b-ba71-82fa300bc4f3
          History

          human spermatozoa,immunocytochemistry,immunoelectron microscopy,mitochondrial membrane potential,mitochondrial progesterone receptor

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