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趋化因子对小鼠排卵后中性粒细胞向阴道迁移的生理调节作用。

Physiologic regulation of postovulatory neutrophil migration into vagina in mice by a C-X-C chemokine(s).

作者信息

Sonoda Y, Mukaida N, Wang J B, Shimada-Hiratsuka M, Naito M, Kasahara T, Harada A, Inoue M, Matsushima K

机构信息

Department of Molecular Pharmacology, Cancer Research Institute, School of Medicine, Kanazawa University, Ishikawa, Japan.

出版信息

J Immunol. 1998 Jun 15;160(12):6159-65.

PMID:9637534
Abstract

Leukocytes, particularly neutrophils, infiltrate into female genital organs after ovulation in both humans and mice. In mice, a female sexual cycle consists of 5 phases: proestrus, estrus, metestrus-1, metestrus-2, and diestrus. Ovulation occurs at estrus; at metestrus-2, a large number of neutrophils infiltrate into the vaginal epithelium accompanied by an increased neutrophil number in vaginal lavage fluid. Concomitantly, concentrations of a functional IL-8 homologue, murine macrophage inflammatory protein (MIP)-2, were increased significantly in vaginal lavage fluid at metestrus-2 as compared with other phases. On the contrary, MIP-2 was not detected in plasma during the whole course of a sexual cycle. Moreover, immunohistochemical analyses demonstrated that MIP-2 protein expression was prominent at the upper layer of the vaginal epithelium at metestrus-2, in contrast to a marginal staining in the vaginal epithelium at proestrus and estrus. These results suggest that a C-X-C chemokine, MIP-2, was produced physiologically in the vaginal epithelium in a sexual cycle-dependent manner. Furthermore, the administration of neutralizing anti-IL-8R homologue Abs at proestrus abrogated leukocyte infiltration into the vagina at metestrus. However, anti-MIP-2 Abs reduced leukocyte influx at metestrus by approximately 50%. Thus, a murine IL-8 homologue, MIP-2, and its related molecules physiologically regulate neutrophil migration into the vagina in a sexual cycle-dependent manner.

摘要

在人类和小鼠中,排卵后白细胞,尤其是中性粒细胞会浸润到雌性生殖器官中。在小鼠中,雌性性周期包括5个阶段:动情前期、动情期、间情期-1、间情期-2和动情后期。排卵发生在动情期;在间情期-2,大量中性粒细胞浸润到阴道上皮,同时阴道灌洗液中的中性粒细胞数量增加。与此相伴的是,与其他阶段相比,在间情期-2时阴道灌洗液中功能性白细胞介素-8同源物——小鼠巨噬细胞炎性蛋白(MIP)-2的浓度显著增加。相反,在整个性周期过程中血浆中未检测到MIP-2。此外,免疫组织化学分析表明,与动情前期和动情期阴道上皮的边缘染色相比,MIP-2蛋白表达在间情期-2时阴道上皮的上层很突出。这些结果表明,一种C-X-C趋化因子MIP-2在性周期依赖性的情况下在阴道上皮中生理性产生。此外,在动情前期给予中和性抗白细胞介素-8受体同源物抗体可消除间情期白细胞向阴道的浸润。然而,抗MIP-2抗体使间情期白细胞流入减少约50%。因此,小鼠白细胞介素-8同源物MIP-2及其相关分子以性周期依赖性的方式生理性调节中性粒细胞向阴道的迁移。

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