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重复给予低剂量脂多糖可诱导小鼠早产:一种用于人类早产及评估药物抗早产治疗能力的模型。

Repeated administration of low-dose lipopolysaccharide induces preterm delivery in mice: a model for human preterm parturition and for assessment of the therapeutic ability of drugs against preterm delivery.

作者信息

Kaga N, Katsuki Y, Obata M, Shibutani Y

机构信息

Toxicology Laboratory, Mochida Pharmaceutical Co., Ltd., Shizuoka, Japan.

出版信息

Am J Obstet Gynecol. 1996 Feb;174(2):754-9. doi: 10.1016/s0002-9378(96)70460-x.

DOI:10.1016/s0002-9378(96)70460-x
PMID:8623817
Abstract

OBJECTIVE

Our purpose was to establish a new animal model for human preterm delivery for assessment of the protective effect of drugs against preterm delivery.

STUDY DESIGN

C3H/HeN, C3H/HeN, and BALB/c female mice impregnated by C3H/HeN, B6D2F1, and B6D2F1 male mice, respectively, were treated intraperitoneally with Escherichia coli lipopolysaccharide (0 to 100 microgram/kg, single dose or repeated doses at 1- to 6-hour intervals) on days 12 through 17 of pregnancy. On day 15 of pregnancy, the C3H/HeN females that had been impregnated by B6D2F1 males and administered lipopolysaccharide were treated intraperitoneally with indomethacin (1000 microgram/kg), ritodrine hydrochloride (1000 microgram/kg), urinary trypsin inhibitor (25 x 10(4) units/kg), or gabexate mesylate (100 mg/kg); preterm or term delivery was recorded for these mice.

RESULTS

C3H/HeN females impregnated by B6D2F1 males revealed the highest (100%) incidence of preterm delivery when the females were treated with 50 microgram/kg lipopolysaccharide twice at a 3-hour interval on day 15 or 17 of pregnancy. Indomethacin and urinary trypsin inhibitor used separately significantly decreased the incidence of preterm delivery, but only urinary trypsin inhibitor, and not any of the other drugs, significantly increased the incidence of term delivery in the mice.

CONCLUSION

A new animal model for investigation of preterm delivery was established, and its usefulness for assessment of the protective effect of drugs against preterm delivery was demonstrated.

摘要

目的

我们的目的是建立一种用于人类早产的新动物模型,以评估药物对早产的保护作用。

研究设计

分别用C3H/HeN、B6D2F1和B6D2F1雄性小鼠使C3H/HeN、C3H/HeN和BALB/c雌性小鼠受孕,在妊娠第12至17天腹腔注射大肠杆菌脂多糖(0至100微克/千克,单次剂量或每隔1至6小时重复给药)。在妊娠第15天,对已被B6D2F1雄性小鼠受孕并给予脂多糖的C3H/HeN雌性小鼠腹腔注射吲哚美辛(1000微克/千克)、盐酸利托君(1000微克/千克)、尿胰蛋白酶抑制剂(25×10⁴单位/千克)或甲磺酸加贝酯(100毫克/千克);记录这些小鼠的早产或足月分娩情况。

结果

当在妊娠第15天或第17天以3小时的间隔对被B6D2F1雄性小鼠受孕的C3H/HeN雌性小鼠两次给予50微克/千克脂多糖时,早产发生率最高(100%)。单独使用吲哚美辛和尿胰蛋白酶抑制剂可显著降低早产发生率,但只有尿胰蛋白酶抑制剂能显著提高小鼠的足月分娩发生率,其他药物均无此作用。

结论

建立了一种用于研究早产的新动物模型,并证明了其在评估药物对早产保护作用方面的实用性。

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