Abstract

Infertility affects one out of every eight couples, with male dysfunction contributing to half of this incidence. The causes of male reproductive failure are usually unknown, though recent attention has focused on environmental toxicants and their effects. Microtubule disrupters - including model compounds (colchicine, taxol) and environmental contaminants (the benomyl metabolite, carbendazim, and the n-hexane metabolite, 2,5-hexanedione) - are male reproductive toxicants which target Sertoli cell microtubules and produce irreversible testicular injury and infertility. Past work using predominantly biochemical and cell biological in vitro approaches has suggested that these toxicants initiate a cascade of events: inhibition of Sertoli cell microtubule-dependent transport leads to decreased seminiferous tubule fluid formation and germ cell death. This working hypothesis is tested in this project with new methods developed to assess Sertoli cell functions in vivo. In preliminary studies, selective infection of rat Sertoli cells was accomplished by in vivo injection of replication-deficient adenovirus into the rete testis. Initial experiments will characterize this new technique, evaluating onset and persistence of adenovirus-directed gene expression. Next, two properties of this adenovirus injection system will be exploited to study the in vivo consequences of Sertoli cell microtubule disruption. First, since adenovirus is known to use microtubule tracks for translocation from the cell periphery to the nucleus, the time required for adenovirus to appear in the Sertoli cell nucleus after rete injection will be used to measure microtubule-dependent transport rates in this target cell. Second, the gene transfer capability of adenovirus will be used to over-express gamma-tubulin or to knock-out kinesin in the Sertoli cell, permitting germ cell viability to be evaluated in the setting of a selective failure of Sertoli cell microtubule-dependent transport. Together, these complimentary approaches will critically examine key steps in the pathogenetic sequence by which microtubule disrupters alter the supportive capacity of Sertoli cells resulting in loss of germ cells and infertility.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
5R01ES008956-05
Application #
6382222
Study Section
Special Emphasis Panel (ZRG4-ALTX-2 (01))
Program Officer
Mcclure, Michael
Project Start
1997-09-01
Project End
2002-08-31
Budget Start
2001-09-01
Budget End
2002-08-31
Support Year
5
Fiscal Year
2001
Total Cost
$268,255
Indirect Cost

  Institution

Name
Brown University
Department
Pathology
Type
Schools of Medicine
DUNS #
001785542
City
Providence
State
RI
Country
United States
Zip Code
02912

  Publications

Fleming, Shawna L; Shank, Peter R; Boekelheide, Kim (2003) gamma-Tubulin overexpression in Sertoli cells in vivo. II: Retention of spermatids, residual bodies, and germ cell apoptosis. Biol Reprod 69:322-30
Fleming, Shawna L; Shank, Peter R; Boekelheide, Kim (2003) gamma-Tubulin overexpression in Sertoli cells in vivo: I. Localization to sites of spermatid head attachment and alterations in Sertoli cell microtubule distribution. Biol Reprod 69:310-21
Boekelheide, Kim; Fleming, Shawna L; Allio, Theresa et al. (2003) 2,5-hexanedione-induced testicular injury. Annu Rev Pharmacol Toxicol 43:125-47
Johnson, Kamin J; Boekelheide, Kim (2002) Dynamic testicular adhesion junctions are immunologically unique. I. Localization of p120 catenin in rat testis. Biol Reprod 66:983-91
Weiss, Bernard (2002) Sexually dimorphic nonreproductive behaviors as indicators of endocrine disruption. Environ Health Perspect 110 Suppl 3:387-91
Johnson, Kamin J; Boekelheide, Kim (2002) Dynamic testicular adhesion junctions are immunologically unique. II. Localization of classic cadherins in rat testis. Biol Reprod 66:992-1000
Boekelheide, K; Fleming, S L; Johnson, K J et al. (2000) Role of Sertoli cells in injury-associated testicular germ cell apoptosis. Proc Soc Exp Biol Med 225:105-15
Johnson, K J; Patel, S R; Boekelheide, K (2000) Multiple cadherin superfamily members with unique expression profiles are produced in rat testis. Endocrinology 141:675-83
Varmuza, S; Jurisicova, A; Okano, K et al. (1999) Spermiogenesis is impaired in mice bearing a targeted mutation in the protein phosphatase 1cgamma gene. Dev Biol 205:98-110