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人胚胎发育中的肺以及肺癌中I和唾液酸化I抗原的分化依赖性表达。

Differentiation-dependent expression of I and sialyl I antigens in the developing lung of human embryos and in lung cancers.

作者信息

Itai S, Nishikata J, Takahashi N, Tanaka O, Matsubara Y, Hasegawa S, Yanai N, Takaoka K, Arii S, Tobe T

机构信息

Department of Clinical Science, Kyoto University, School of Medicine, Japan.

出版信息

Cancer Res. 1990 Dec 1;50(23):7603-11.

PMID:1979246
Abstract

The localization of two carbohydrate antigens, I and sialyl I antigens, in the lungs of developing human embryos was investigated using specific monoclonal antibodies and compared with the distribution patterns of the known embryonic antigen, stage-specific embryonic antigen-1 (Lex hapten). When the future bronchi were actively developing from the bronchial buds in the lungs of 50- to 53-day-old embryos, the immature bronchial bud cells were I-, Lex+, while the fully differentiated epithelial cells of the larger bronchus were I+, Lex-. When the bronchiolar bud cells matured into bronchiolar epithelial cells in the lung of a 12-week-old embryo, the immature bronchiolar bud cells were I-,Lex+, while the fully differentiated epithelial cells of the bronchioles were I+,Lex-. Sialylated forms of the antigens finally appeared in the lungs of 18-week-old embryos, when the terminal bud cells actively proliferated and underwent the differentiation process into epithelial cells of alveoli and alveolar ducts. The immature terminal bud cells at this stage were I-, sialyl I-, Lex+, sialyl Lex-i+, while the fully differentiated alveolar epithelial cells were I+, sialyl I+, Lex-, sialyl Lex-i-. After 8 months, the flattened mature alveolar epithelial cells were strongly positive for both I and sialyl I antigens, the strong expression of which continued after birth and even into the adult stage. These distribution patterns indicate that the I and sialyl I antigens are specific markers for the differentiated type cells in each stage of development, while Lex and related embryonic antigens were specific to the immature bud cells in every stage. The above-described differentiation-dependent expression patterns of these antigens seem to be reflected in the distribution of these antigens in human lung cancers, i.e., I and sialyl I antigens were expressed in lung cancer cells more weakly than in normal lung cells, while the Lex and sialyl Lex-i were expressed in cancer cells much more strongly than in normal lung cells. This was further reflected in the serum levels of these antigens in the patients with respiratory disorders. The distribution pattern of the serum levels of these antigens in patients with lung cancers showed sialyl Lex-i greater than sialyl I, indicating that these serum antigens originated from the lung cancer lesion where sialyl Lex-i is much more dominant than sialyl I antigen.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

利用特异性单克隆抗体研究了两种碳水化合物抗原,即I抗原和唾液酸化I抗原,在发育中的人类胚胎肺中的定位,并与已知胚胎抗原阶段特异性胚胎抗原-1(Lex半抗原)的分布模式进行了比较。在50至53日龄胚胎肺中,当未来的支气管从支气管芽中积极发育时,未成熟的支气管芽细胞为I-、Lex+,而较大支气管的完全分化上皮细胞为I+、Lex-。在12周龄胚胎肺中,当细支气管芽细胞成熟为细支气管上皮细胞时,未成熟的细支气管芽细胞为I-、Lex+,而细支气管的完全分化上皮细胞为I+、Lex-。抗原的唾液酸化形式最终出现在18周龄胚胎的肺中,此时终末芽细胞积极增殖并经历分化过程成为肺泡和肺泡管的上皮细胞。此阶段未成熟的终末芽细胞为I-、唾液酸化I-、Lex+、唾液酸化Lex-i+,而完全分化的肺泡上皮细胞为I+、唾液酸化I+、Lex-、唾液酸化Lex-i-。8个月后,扁平的成熟肺泡上皮细胞对I抗原和唾液酸化I抗原均呈强阳性,其强表达在出生后甚至成年期持续存在。这些分布模式表明,I抗原和唾液酸化I抗原是发育各阶段分化型细胞的特异性标志物,而Lex及相关胚胎抗原在每个阶段均特异性地存在于未成熟的芽细胞中。上述这些抗原依赖分化的表达模式似乎反映在它们在人类肺癌中的分布情况,即I抗原和唾液酸化I抗原在肺癌细胞中的表达比在正常肺细胞中弱,而Lex和唾液酸化Lex-i在癌细胞中的表达比在正常肺细胞中强得多。这在呼吸系统疾病患者这些抗原的血清水平中进一步得到体现。肺癌患者这些抗原血清水平的分布模式显示唾液酸化Lex-i大于唾液酸化I,表明这些血清抗原源自唾液酸化Lex-i比唾液酸化I抗原更占优势的肺癌病灶。(摘要截断于400字)

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