Literature DB >> 12887277

Dose-response of RAG2-/-/gammac-/- mice to busulfan in preparation for spermatogonial transplantation.

A E Moisan1, R A Foster, K J Betteridge, A C Hahnel.   

Abstract

Practical applications of spermatogonial transplantation require good rates of colonization by the donor cells. Recipient testes are usually depleted of competing endogenous spermatogonia by administration of 32-44 mg busulfan kg(-1) body weight before transplantation. However, it is not clear that this is the optimum dose, especially for immunodeficient mice. In the present study, the response of adult RAG2(-/-)/gamma(c)(-/-) (RAG2) male mice to treatment with 10-50 mg busulfan kg(-1) body weight was determined in terms of mortality rates, testicular masses and histology, and colonization of seminiferous tubules by transplanted spermatogonia. Mortality increased from 0 to 50% at doses between 20 mg busulfan kg(-1) and 40 mg busulfan kg(-1), whereas the maximum effects on testicular mass and histology were observed at 20 mg busulfan kg(-1). Colonization of testes by genetically marked spermatogonia after treatment of mice with 20 mg busulfan kg(-1) was equivalent to rates previously reported in recipients treated with 32-44 mg busulfan kg(-1). Thus, 20 mg busulfan kg(-1) appears to be the optimum dose for preparing RAG2 mice for spermatogonial transplantation. However, because the steepness of the dose-response curves indicates that direct administration of busulfan is not ideal for this purpose, 15 mg busulfan kg(-1) was administered to pregnant females at various times between day 10.5 and day 16.5 of gestation to determine whether this would deplete the number of germ cells in male offspring. Although there were large variations in testicular mass and histology, no mortality was observed and administration of busulfan at day 10.5 or 12.5 after mating delayed initiation of spermatogenesis, indicating that prenatal administration of busulfan combined with neonatal transplantation might be an effective method for further increasing rates of colonization by donor spermatogonia.

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Year:  2003        PMID: 12887277     DOI: 10.1530/rep.0.1260205

Source DB:  PubMed          Journal:  Reproduction        ISSN: 1470-1626            Impact factor:   3.906


  7 in total

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4.  Optimal dose of busulfan for depleting testicular germ cells of recipient mice before spermatogonial transplantation.

Authors:  De-Zhi Wang; Xin-Hua Zhou; Yu-Lin Yuan; Xin-Min Zheng
Journal:  Asian J Androl       Date:  2009-12-14       Impact factor: 3.285

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6.  Testicular Busulfan Injection in Mice to Prepare Recipients for Spermatogonial Stem Cell Transplantation Is Safe and Non-Toxic.

Authors:  YuSheng Qin; Ling Liu; YaNan He; Chen Wang; MingYuan Liang; XiaoLi Chen; HaiSheng Hao; Tong Qin; XueMing Zhao; Dong Wang
Journal:  PLoS One       Date:  2016-02-12       Impact factor: 3.240

7.  Establishing a nonlethal and efficient mouse model of male gonadotoxicity by intraperitoneal busulfan injection.

Authors:  Yun Xie; Cun-Can Deng; Bin Ouyang; Lin-Yan Lv; Jia-Hui Yao; Chi Zhang; Hai-Cheng Chen; Xiao-Yan Li; Xiang-Zhou Sun; Chun-Hua Deng; Gui-Hua Liu
Journal:  Asian J Androl       Date:  2020 Mar-Apr       Impact factor: 3.285

  7 in total

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