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妊娠期垂体:69例临床病理及免疫组化研究

The pituitary gland in pregnancy: a clinicopathologic and immunohistochemical study of 69 cases.

作者信息

Scheithauer B W, Sano T, Kovacs K T, Young W F, Ryan N, Randall R V

机构信息

Division of Pathology, Mayo Clinic, Rochester, MN 55905.

出版信息

Mayo Clin Proc. 1990 Apr;65(4):461-74. doi: 10.1016/s0025-6196(12)60946-x.

Abstract

A histologic and immunocytochemical study of 69 autopsy-obtained pituitaries from women who died during pregnancy, after abortion, or in the postpartum period revealed an accumulation of large chromophobic to slightly acidophilic and periodic acid-Schiff-negative pregnancy cells that were immunoreactive for prolactin but not for other pituitary hormones. This increase in the number of prolactin cells was confirmed by cell counts. Thus, pregnancy cells are capable of prolactin production. The finding of mitotic figures in such cells supports the view that they arise by multiplication from preexisting prolactin cells. With use of "mirror section" techniques, no mammosomatotrophs (cells immunoreactive for growth hormone and prolactin) were identified. Hyperplasia of prolactin cells was evident at 1 month of pregnancy and gradually disappeared within several months after delivery or abortion; the process of involution seemed to be retarded in the one lactating patient investigated. In some pituitaries, the accumulation of prolactin cells was so extensive that the hyperplastic foci resembled microadenomas. Another striking change in the pituitaries of pregnant women was appreciable reduction of immunostaining of gonadotropic cells, a process that was reversible as soon as 1 month after delivery. Among the 69 pituitaries studied, 8 noninvasive microadenomas (12%) were encountered (7 contained prolactin only and 1 was plurihormonal). Prolactin-producing adenomas were no more numerous or larger than were similar tumors encountered in nonpregnant women or normal men; thus, pregnancy neither initiates formation of pituitary adenomas nor accelerates their growth. In the pituitaries that harbored prolactin-producing adenomas, massive pregnancy cell hyperplasia was evident outside the tumor; thus, prolactin production by adenoma cells did not seem to suppress the proliferation of prolactin-containing pregnancy cells.

摘要

一项对69例在孕期、流产后或产后死亡的女性尸检获得的垂体进行的组织学和免疫细胞化学研究显示,存在大量嫌色至轻度嗜酸性且过碘酸-希夫反应阴性的妊娠细胞聚集,这些细胞对催乳素呈免疫反应,而对其他垂体激素无反应。通过细胞计数证实了催乳素细胞数量的增加。因此,妊娠细胞能够产生催乳素。在这些细胞中发现有丝分裂象支持了它们是由预先存在的催乳素细胞增殖产生的观点。使用“镜像切片”技术,未发现乳腺生长激素细胞(对生长激素和催乳素呈免疫反应的细胞)。妊娠1个月时催乳素细胞增生明显,在分娩或流产后数月内逐渐消失;在所研究的一名哺乳期患者中, involution过程似乎有所延迟。在一些垂体中,催乳素细胞的聚集非常广泛,以至于增生灶类似微腺瘤。孕妇垂体的另一个显著变化是促性腺细胞免疫染色明显减少,这一过程在分娩后1个月内即可逆转。在研究的69个垂体中,发现了8个非侵袭性微腺瘤(12%)(7个仅含催乳素,1个为多激素性)。产生催乳素的腺瘤在数量或大小上并不比非妊娠女性或正常男性中遇到的类似肿瘤更多或更大;因此,妊娠既不会引发垂体腺瘤的形成,也不会加速其生长。在含有产生催乳素腺瘤的垂体中,肿瘤外可见大量妊娠细胞增生;因此,腺瘤细胞产生催乳素似乎并未抑制含催乳素妊娠细胞的增殖。

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