Abstract

In vivo sperm motility alterations occur in two stages; motility initiation during epididymal transit and transition to hyperactivated motility within the female reproductive tract. We have demonstrated previously that ejaculated primate sperm contain the serine/threonine PP-1, its endogenous regulators and that treatment of human sperm with the cell-permeable protein phosphatase inhibitor calyculin-a (CL-A) stimulates motility. The objectives of this study were to determine macaque caput and caudal epididymal sperm PP activity, caput and caudal epididymal sperm motility following CL-A treatment, and PP activity of ejaculated sperm treated with dibutyryl cAMP (dbcAMP) and caffeine which stimulates hyperactivated motility. Protein phosphatase activity was determined using 32P-labeled phosphorylase-` in the absence of divalent cations. Motility analysis of epididymal sperm was conducted using a computer-assisted motility analysis system following sperm treatment with 0, 10, 20, 50 or 100 nM CL-A for 10 min. Macaque caput epididymal sperm sonicates contained 4-6 fold more PP activity in comparison to caudal epididymal sperm sonicates. Both caput and caudal epididymal sperm sonicates contained heat-stable PP inhibitor activity as well as Mg-ATP dependent glycogen synthase kinase-3 activity. Treatment of caput epididymal sperm with CL-A increased the percent of motile sperm in a dose-dependent manner from 9% (0 nM CL-A) to 30% (100 nM CL-A) whereas CL-A did not influence the percent of motile caudal epididymal sperm. Treatment of in vitro-capacitated macaque sperm with dbcAMP and caffeine for 1 hr resulted in a significant decrease (P < 0.05) in protein phosphatase activity in comparison to nontreated in vitro-capacitated sperm (1.30 q 0.32 and 2.04 q 0.19 x 10 -2 nM/min/10 6 sperm, respectively). These results implicate PP in regulating motility and begin to address mechanisms which control motility initiation of epididymal sperm and the transition to hyperactivated motility of capacitated sperm.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Primate Research Center Grants (P51)
Project #
5P51RR000163-37
Application #
5219783
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
37
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Okoye, Afam A; Hansen, Scott G; Vaidya, Mukta et al. (2018) Early antiretroviral therapy limits SIV reservoir establishment to delay or prevent post-treatment viral rebound. Nat Med 24:1430-1440
Jensen, Jeffrey T; Hanna, Carol; Mishler, Emily et al. (2018) Effect of menstrual cycle phase and hormonal treatments on evaluation of tubal patency in baboons. J Med Primatol 47:40-45
Toro, C A; Aylwin, C F; Lomniczi, A (2018) Hypothalamic epigenetics driving female puberty. J Neuroendocrinol 30:e12589
Bulgarelli, Daiane L; Ting, Alison Y; Gordon, Brenda J et al. (2018) Development of macaque secondary follicles exposed to neutral red prior to 3-dimensional culture. J Assist Reprod Genet 35:71-79
Prola-Netto, Joao; Woods, Mark; Roberts, Victoria H J et al. (2018) Gadolinium Chelate Safety in Pregnancy: Barely Detectable Gadolinium Levels in the Juvenile Nonhuman Primate after in Utero Exposure. Radiology 286:122-128
Moccetti, Federico; Brown, Eran; Xie, Aris et al. (2018) Myocardial Infarction Produces Sustained Proinflammatory Endothelial Activation in Remote Arteries. J Am Coll Cardiol 72:1015-1026
Blue, Steven W; Winchell, Andrea J; Kaucher, Amy V et al. (2018) Simultaneous quantitation of multiple contraceptive hormones in human serum by LC-MS/MS. Contraception 97:363-369
Jeon, Sookyoung; Li, Qiyao; Rubakhin, Stanislav S et al. (2018) 13C-lutein is differentially distributed in tissues of an adult female rhesus macaque following a single oral administration: a pilot study. Nutr Res :
Slayden, Ov Daniel; Friason, Francis Kathryn E; Bond, Kise Rosen et al. (2018) Hormonal regulation of oviductal glycoprotein 1 (OVGP1; MUC9) in the rhesus macaque cervix. J Med Primatol 47:362-370
Dissen, G A; Adachi, K; Lomniczi, A et al. (2017) Engineering a gene silencing viral construct that targets the cat hypothalamus to induce permanent sterility: An update. Reprod Domest Anim 52 Suppl 2:354-358

Showing the most recent 10 out of 492 publications