人胎儿胰腺中的免疫细胞——对糖尿病和器官培养的发育免疫内分泌学的贡献。

Anatomischer Anzeiger Pub Date : 1990-01-01
H Hahn von Dorsche, K Fält
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引用次数: 0

摘要

研究对象为103例妊娠10 ~ 26周的人胎儿胰腺组织。其中14名母亲患有胰岛素依赖型糖尿病(IDDM),其中33名样本在培养前后进行了检查。取3例发育第14周的胎儿(无代谢障碍的母亲),在电镜下观察。淋巴细胞在组织内的分布通常是不规则的。在发育的第12周,还可以发现3到5个淋巴细胞的群,从第14周开始出现更大的群(10到15个淋巴细胞)。将这些定量结果与胎儿早期胰岛器官发育的3个阶段联系起来,可以看出,从发育第10周到第26周,淋巴细胞数量增加。这一点的意义将与免疫系统的发展联系起来讨论。鉴于考虑将胎儿胰腺组织移植作为IDDM的治疗,这意味着在发育第14周之前,免疫原性可能相对较低。胸腺分化在第17周前未完成,淋巴结和脾脏分化持续到第20 ~ 23周。虽然IgG抗体已经在第8周左右通过胎盘屏障转移,但这种通量直到第32周才达到最大值。胎儿体内的内源性抗体合成直到第18周才开始。母亲在胎儿发育期间(第10至26周)的IDDM不会增加胰腺的淋巴细胞数量。这也适用于达到相同发育阶段后培养14天的组织。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immunocytes in the human fetal pancreas--a contribution to developmental immunoendocrinology concerning diabetes mellitus and organ cultivation.

The studies were performed on 103 samples of human fetal pancreas tissue (10th to 26th week of gestation). Of the mothers, 14 had insulin dependent type I diabetes mellitus (IDDM), and 33 of the samples were examined before and after cultivation for 14 days. 3 samples taken from fetuses in the 14th week of development (mothers without metabolic disorders) were examined in the electron microscope. Lymphocytes are generally irregularly distributed within the tissue. Groups of 3 to 5 lymphocytes are found in addition in the 12th week of development, and larger clusters (10 to 15 lymphocytes) appear from the 14th week onward. Relating these quantitative results to the 3 phases of early fetal islet organ development, it can be seen that lymphocyte numbers increase from the 10th to the 26th week of development. The significance of this is discussed in connection with the development of the immune system. In view of the contemplated transplantation of fetal pancreas tissue as treatment for IDDM, it means that a relatively low immunogenicity can be expected up to the 14th week of development. Thymic differentiation is not complete before the 17th week, and differentiation of the lymph nodes and spleen continues until weeks 20 to 23. Although IgG antibodies are transferred across the placental barrier already in about the 8th week, this flux does not reach its maximum until the 32nd week. Endogenous antibody synthesis in the fetus does not start until the 18th week. IDDM of the mother during fetal development (10th to 26th week) does not increase the lymphocyte number in the pancreas. This also applies to tissue that has been cultivated for 14 days after reaching the same stage of development.

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