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先天性恶性贫血患者的胃液中不含有免疫反应性内因子分子:对三个发病年龄各异的家族进行的研究,其中包括一名成年后首次确诊的患者。

Gastric juice in congenital pernicious anemia contains no immunoreactive intrinsic factor molecule: study of three kindreds with variable ages at presentation, including a patient first diagnosed in adulthood.

作者信息

Carmel R

出版信息

Am J Hum Genet. 1983 Jan;35(1):67-77.

Abstract

The mechanism responsible for the isolated intrinsic factor deficiency in congenital pernicious anemia is unknown. A new second-antibody radioimmunoassay capable of recognizing intrinsic factor independent of the molecule's ability to bind added cobalamin was used to study six patients from three kindreds with this disorder. One of the patients was first diagnosed at age 23 because of unusual circumstances in her case; yet the other patients also demonstrated great age variability at presentation of this presumably congenital disorder, even within the same kindred. The radioimmunoassay failed to detect immunoreactive intrinsic factor in any of the six patients, suggesting that elaboration of an abnormal molecule was not the pathogenetic mechanism. An unexpected incidental finding, contrasting with this observation in congenital pernicious anemia, was immunologic evidence that a previously described patient with familial R binder deficiency clearly elaborated an abnormal R binder molecule.

摘要

先天性恶性贫血中单纯内因子缺乏的发病机制尚不清楚。一种新的第二抗体放射免疫测定法,能够识别与添加钴胺素结合能力无关的内因子,用于研究来自三个家族的六名患有这种疾病的患者。其中一名患者因特殊情况在23岁时首次被诊断;然而,其他患者在这种可能是先天性疾病出现时也表现出很大的年龄差异,即使在同一家族中也是如此。放射免疫测定法未能在这六名患者中的任何一人中检测到免疫反应性内因子,这表明异常分子的产生不是发病机制。与先天性恶性贫血中的这一观察结果形成对比的一个意外偶然发现是,免疫证据表明,先前描述的一名患有家族性R结合蛋白缺乏症的患者明显产生了一种异常的R结合蛋白分子。

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引用本文的文献

本文引用的文献

1
Juvenile pernicious anemia.青少年恶性贫血
Pediatrics. 1951 Jul;8(1):88-106.
4
PERNICIOUS ANEMIA IN CHILDHOOD.儿童恶性贫血
N Engl J Med. 1965 May 13;272:981-6. doi: 10.1056/NEJM196505132721901.
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IN VITRO ASSAY FOR HUMAN INTRINSIC FACTOR.人内因子的体外测定
J Clin Invest. 1963 Sep;42(9):1443-58. doi: 10.1172/JCI104829.
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Familial juvenile pernicious anaemia: a study of the hereditary basis of pernicious anaemia.
Br J Haematol. 1963 Jan;9:1-12. doi: 10.1111/j.1365-2141.1963.tb05435.x.

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