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抗转钴胺素II循环抗体导致维生素B12滞留于血液中。

Circulating antibody to transcobalamin II causing retention of vitamin B12 in the blood.

作者信息

Carmel R, Tatsis B, Baril L

出版信息

Blood. 1977 Jun;49(6):987-1000.

PMID:861380
Abstract

A patient with recurrent pulmonary abscess, weight loss, and alcoholism was found to have extremely high serum vitamin B12 and unsaturated vitamin B12-binding capacity (UBBC) levels. While transcobalamin (TC) II was also increased, most of his UBBC was due to an abnormal binding protein which carried greater than 80% of the endogenous vitamin B12 and was not found in his saliva, granulocytes, or urine. This protein was shown to be a complex of TC II and a circulating immunoglobulin (IgGkappa and IgGlambda). Each IgG molecule appeared to bind two TC II molecules. The reacting site did not interfere with the ability of TC II to bind vitamin B12, but did interfere with its ability to transfer the vitamin to cells in vitro. The site was not identical to that reacting with anti-human TC II antibody produced in rabbits. Because of this abnormal complex, 57Co-vitamin B12 injected intravenously was cleared slowly by the patient. However, no metabolic evidence for vitamin B12 deficiency was demonstrable, although the patient initially had megaloblastic anemia apparently due to folate deficiency. The course of the vitamin B12-binding abnormalities was followed over 4 yr and appeared to fluctuate with the status of the patient's illness. The IgG-TC II complex resembled one induced in some patients with pernicious anemia by intensive treatment with long-acting vitamin B12 preparations. The mechanism of induction of the antibody formation in our patient is unknown.

摘要

一名患有复发性肺脓肿、体重减轻且酗酒的患者,血清维生素B12及不饱和维生素B12结合能力(UBBC)水平极高。虽然转钴胺素(TC)II也有所升高,但他的大部分UBBC是由一种异常结合蛋白所致,该蛋白携带了超过80%的内源性维生素B12,且在其唾液、粒细胞或尿液中未被发现。这种蛋白被证明是TC II与循环免疫球蛋白(IgGκ和IgGλ)的复合物。每个IgG分子似乎能结合两个TC II分子。反应位点并不干扰TC II结合维生素B12的能力,但确实会干扰其在体外将维生素转运至细胞的能力。该位点与兔体内产生的抗人TC II抗体的反应位点不同。由于这种异常复合物,静脉注射的57Co-维生素B12在患者体内清除缓慢。然而,尽管患者最初因叶酸缺乏出现巨幼细胞贫血,但未发现维生素B12缺乏的代谢证据。对维生素B12结合异常情况进行了4年的跟踪,其似乎随患者病情状况而波动。IgG-TC II复合物类似于一些恶性贫血患者在接受长效维生素B12制剂强化治疗后诱导产生的复合物。我们患者体内抗体形成的诱导机制尚不清楚。

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