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胎儿期和围生期人肾上腺皮质的增殖与凋亡:对生长和重塑的影响

Proliferation and apoptosis in the human adrenal cortex during the fetal and perinatal periods: implications for growth and remodeling.

作者信息

Spencer S J, Mesiano S, Lee J Y, Jaffe R B

机构信息

Reproductive Endocrinology Center, Department of Obstetrics, Gynecology, and Reproductive Sciences, University of California, San Francisco, 94143-0556, USA.

出版信息

J Clin Endocrinol Metab. 1999 Mar;84(3):1110-5. doi: 10.1210/jcem.84.3.5513.

Abstract

After 10-15 weeks of gestation, the human fetal adrenal cortex undergoes rapid growth due to enlargement of a specialized cortical compartment known as the fetal zone (FZ). Soon after birth, the FZ regresses and the adult zonation pattern develops at least in part from cells derived from the persistent definitive zone (DZ), a thin layer of tightly packed cells surrounding the FZ. We postulated that growth of the fetal adrenal cortex involves zone-specific cellular hyperplasia, whereas the postnatal involution of the FZ is due to apoptosis. Therefore, we investigated the pattern of cellular proliferation and death in the FZ and DZ of the human fetal and postnatal adrenal cortex using immunohistochemical staining for proliferating cell nuclear antigen as a marker of mitosis and in situ detection of DNA fragmentation as a marker of apoptosis. Between 10-14 weeks' gestation, the mitotic indexes (percentage of proliferating cell nuclear antigen-positive cells) in the DZ (26.46 +/- 2.95%) and in the FZ (21.26 +/- 2.57%) were not significantly different. Between 15-20 weeks gestation, the mitotic index increased significantly (P < 0.05) in both zones (FZ, 33.84 +/- 5.21%; DZ, 67.45 +/- 7.58%) relative to levels before 15 weeks. This increase persisted between 21-24 weeks gestation (FZ, 39.5 +/- 4.22%; DZ, 58.63 +/- 6.83%). Interestingly, after 14 weeks, the mitotic index of the DZ was significantly greater (P < 0.05) than that of the FZ. In adrenal specimens obtained from infants born prematurely and treated in utero with glucocorticoid, the mitotic indexes in the FZ and DZ were significantly decreased. At all stages of gestation, no apoptotic nuclei were detected in the DZ. However, scattered apoptotic nuclei were detected in the central portions of the FZ. The number of apoptotic nuclei in the inner FZ increased with advancing gestation and was maximal during the first postnatal month. To identify factors that may regulate apoptosis, primary cultures of midgestation FZ cells were treated with activin A and transforming growth factor-beta (TGFbeta). Activin A and TGFbeta both induced apoptotic cell death, as assessed by internucleosomal DNA cleavage (DNA laddering). Induction of apoptosis by activin A was prevented by concomitant addition of follistatin, an activin-binding protein. Taken together, these data indicate that 1) growth of the human fetal adrenal cortex involves cellular hyperplasia, mainly in the DZ and to a lesser extent in the FZ, which is probably dependent on ACTH; and 2) apoptosis occurs predominantly in the inner cortical compartment and may be responsible for the rapid regression of the FZ after birth, a process that may be regulated by activin A and/or TGFbeta.

摘要

妊娠10 - 15周后,由于一个称为胎儿带(FZ)的特殊皮质区室增大,人类胎儿肾上腺皮质迅速生长。出生后不久,胎儿带退化,成人的分区模式至少部分由源自持久的定区(DZ)的细胞发育而来,定区是围绕胎儿带的一层紧密排列的薄细胞层。我们推测胎儿肾上腺皮质的生长涉及特定区域的细胞增生,而胎儿带出生后的退化是由于细胞凋亡。因此,我们使用增殖细胞核抗原免疫组化染色作为有丝分裂的标志物,以及DNA片段原位检测作为细胞凋亡的标志物,研究了人类胎儿及出生后肾上腺皮质中胎儿带和定区的细胞增殖和死亡模式。在妊娠10 - 14周之间,定区(26.46±2.95%)和胎儿带(21.26±2.57%)的有丝分裂指数(增殖细胞核抗原阳性细胞的百分比)无显著差异。在妊娠15 - 20周之间,相对于15周前的水平,两个区域的有丝分裂指数均显著增加(P<0.05)(胎儿带,33.84±5.21%;定区,67.45±7.58%)。这种增加在妊娠21 - 24周之间持续存在(胎儿带,39.5±4.22%;定区,58.63±6.83%)。有趣的是,14周后,定区的有丝分裂指数显著高于胎儿带(P<0.05)。在早产并在子宫内接受糖皮质激素治疗的婴儿的肾上腺标本中,胎儿带和定区的有丝分裂指数显著降低。在妊娠的所有阶段,定区均未检测到凋亡细胞核。然而,在胎儿带的中央部分检测到散在的凋亡细胞核。胎儿带内层的凋亡细胞核数量随妊娠进展而增加,并在出生后的第一个月达到最大值。为了确定可能调节细胞凋亡的因素,用激活素A和转化生长因子β(TGFβ)处理妊娠中期胎儿带细胞的原代培养物。激活素A和TGFβ均诱导凋亡性细胞死亡,通过核小体间DNA裂解(DNA梯状条带)评估。激活素A诱导的细胞凋亡可通过同时添加激活素结合蛋白卵泡抑素来预防。综上所述,这些数据表明:1)人类胎儿肾上腺皮质的生长涉及细胞增生,主要发生在定区,胎儿带中程度较轻,这可能依赖于促肾上腺皮质激素;2)细胞凋亡主要发生在皮质内层区室,可能是出生后胎儿带迅速退化的原因,这一过程可能受激活素A和/或TGFβ调节。

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