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小鼠精子发生对米格鲁司他的敏感性是一种数量性状:一项药物遗传学研究。

The sensitivity of murine spermiogenesis to miglustat is a quantitative trait: a pharmacogenetic study.

作者信息

Bone Wilhelm, Walden Charlotte M, Fritsch Martin, Voigtmann Ulrike, Leifke Eckhard, Gottwald Ulrich, Boomkamp Stephanie, Platt Frances M, van der Spoel Aarnoud C

机构信息

Schering AG, Müllerstr. 178, 13342 Berlin, Germany.

出版信息

Reprod Biol Endocrinol. 2007 Jan 22;5:1. doi: 10.1186/1477-7827-5-1.

Abstract

BACKGROUND

A major event in the post-meiotic development of male germ cells is the formation of the acrosome. This process can be perturbed in C57BL/6 mice by administration of the small molecule miglustat (N-butyldeoxynojirimycin, NB-DNJ). The miglustat-treated mice produce morphologically abnormal spermatozoa that lack acrosomes and are poorly motile. In C57BL/6 mice, miglustat can be used to maintain long-term reversible infertility. In contrast, when miglustat was evaluated in normal men, it did not affect spermatogenesis. To gain more insight into this species difference we have now evaluated the reproductive effects of miglustat in rabbits, in multiple mouse strains and in interstrain hybrid mice.

METHODS

Male mice of 18 inbred strains were administered miglustat orally or via miniosmotic pumps. Rabbits were given the compound in their food. Fourth-generation interstrain hybrid mice, bred from C57BL/6 and FVB/N mice (which differ in their response to miglustat), also received the drug. Data on fertility (natural mating), sperm motility and morphology, acrosome status, and serum drug levels were collected.

RESULTS

In rabbits the drug did not induce aberrations of sperm shape or motility, although the serum level of miglustat in rabbits far exceeded the level in C57BL/6 mice (8.4 microM and 0.5 microM, respectively). In some strains of the Swiss and Castle lineages of inbred mice miglustat did not cause infertility, severe morphological sperm aberrations or reduced sperm motility. In these strains miglustat only had milder effects. However, miglustat strongly disturbed acrosome and sperm nucleus development in AKR/J and BALB/c mice and in a number of C57BL/6-related strains. The consequences of drug administration in the interstrain hybrid mice were highly variable. Judging by the number of grossly abnormal spermatozoa, these genetically heterogeneous mice displayed a continuous range of intermediate responses, distinct from either of their parental strains.

CONCLUSION

The effects of miglustat on spermatogenesis in mice are strain-dependent, while in rabbits the drug is ineffective. Evaluation of interstrain hybrid mice indicated that the sensitivity of spermatogenesis to miglustat is a quantitative trait. These studies pave the way for identifying the genetic factors underlying the strain/species differences in the effect of miglustat.

摘要

背景

雄性生殖细胞减数分裂后发育过程中的一个主要事件是顶体的形成。在C57BL/6小鼠中,给予小分子药物米格列醇(N-丁基脱氧野尻霉素,NB-DNJ)会干扰这一过程。经米格列醇处理的小鼠产生形态异常的精子,这些精子缺乏顶体且运动能力差。在C57BL/6小鼠中,米格列醇可用于维持长期可逆性不育。相比之下,在正常男性中评估米格列醇时,它对精子发生没有影响。为了更深入了解这种物种差异,我们现在评估了米格列醇对兔子、多种小鼠品系和品系间杂交小鼠的生殖影响。

方法

给18个近交系雄性小鼠口服米格列醇或通过微型渗透泵给药。给兔子在食物中添加该化合物。由C57BL/6和FVB/N小鼠(它们对米格列醇的反应不同)培育的第四代品系间杂交小鼠也接受了该药物。收集了关于生育力(自然交配)、精子活力和形态、顶体状态以及血清药物水平的数据。

结果

在兔子中,该药物未诱导精子形状或活力异常,尽管兔子血清中的米格列醇水平远远超过C57BL/6小鼠中的水平(分别为8.4微摩尔和0.5微摩尔)。在一些瑞士和卡斯尔系近交小鼠品系中,米格列醇不会导致不育、严重的精子形态异常或精子活力降低。在这些品系中,米格列醇只有较轻微的影响。然而,米格列醇严重干扰了AKR/J和BALB/c小鼠以及一些与C57BL/6相关品系中的顶体和精子细胞核发育。在品系间杂交小鼠中给药的后果差异很大。从严重异常精子的数量来看,这些基因异质的小鼠表现出一系列连续的中间反应,与它们的任何一个亲本品系都不同。

结论

米格列醇对小鼠精子发生的影响具有品系依赖性,而在兔子中该药物无效。对品系间杂交小鼠的评估表明,精子发生对米格列醇的敏感性是一个数量性状。这些研究为确定米格列醇作用中品系/物种差异背后的遗传因素铺平了道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c330/1794412/ba5a4ddd52a9/1477-7827-5-1-1.jpg

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