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显性致死和可遗传易位方法的比较。

Comparison of dominant lethal and heritable translocation methodologies.

作者信息

Anderson D, Hodge M C, Palmer S, Purchase I F

出版信息

Mutat Res. 1981 Dec;85(6):417-29. doi: 10.1016/0165-1161(81)90243-0.

Abstract

Groups of male Alderly Park mice of proven fertility were dosed by gavage for 5 consecutive days per week for 8 weeks or 5 consecutive days only with 100 or 150 mg/kg body weight ethyl methanesulphonate (EMS) or by intraperitoneal injection once a week for 8 weeks or once only with 500 mg/kg shikimic acid. Animals dosed in this manner were compared in the dominant lethal and heritable translocation assays. Animals were mated for 2 consecutive weeks following the 8-week treatment and for 8 consecutive weeks after the 1-week treatment: regimes which were thus non-specific and specific respectively for the stages of spermatogenesis. An additional method of measuring dominant lethality involving counting uterine scars after weaning (Soares (1972) Mutation Res., 16, 425-427) was used and also compared with the conventional method. EMS was clearly confirmed as a mutagen but this was not the case for shikimic acid. For screening purposes the dominant lethal 8-week mating assay was much more efficient in return for the same effort for detecting mutagenic responses than an 8-week mating heritable translocation assay, since the induction of dominant lethal effects paralleled the induction of heritable translocations. 8-week treatment with EMS showed increased dominant lethality but severely reduced fertility and the small numbers of male offspring born made potential heritable effects difficult to assess. The 1-week treatment with EMS produced both dominant lethal and heritable effects. Soares' method can be useful for determining dominant lethal effects in a heritable translocation assay. The "sieving" method of mating to determine partial and total sterility questions the necessity for a negative control in a heritable translocation study.

摘要

选用已证实具有生育能力的老年雄性阿尔德利公园小鼠,每周连续5天经口灌胃,持续8周,给予100或150mg/kg体重的甲磺酸乙酯(EMS),或仅连续5天给予该剂量;或每周腹腔注射1次,持续8周,给予500mg/kg的莽草酸,或仅注射1次。对以这种方式给药的动物进行显性致死和可遗传易位试验,并进行比较。在8周治疗后,动物连续交配2周;在1周治疗后,动物连续交配8周:因此,这些方案分别对精子发生阶段具有非特异性和特异性。还采用了另一种测量显性致死率的方法,即在断奶后计数子宫瘢痕(Soares(1972年),《突变研究》,第16卷,第425 - 427页),并与传统方法进行比较。EMS被明确确认为诱变剂,但莽草酸并非如此。出于筛选目的,在检测诱变反应付出相同努力的情况下,8周显性致死交配试验比8周交配可遗传易位试验效率更高,因为显性致死效应的诱导与可遗传易位的诱导平行。用EMS进行8周治疗显示显性致死率增加,但生育力严重降低,出生的雄性后代数量很少,使得潜在的可遗传效应难以评估。用EMS进行1周治疗产生了显性致死和可遗传效应。Soares的方法可用于在可遗传易位试验中确定显性致死效应。用于确定部分和完全不育的交配“筛选”方法对可遗传易位研究中阴性对照的必要性提出了质疑。

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