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副肿瘤性抗神经元核IgG自身抗体(I型)将抗原定位于小细胞肺癌中。

Paraneoplastic anti-neuronal nuclear IgG autoantibodies (type I) localize antigen in small cell lung carcinoma.

作者信息

Kiers L, Altermatt H J, Lennon V A

机构信息

Department of Neurology, Mayo Clinic, Rochester, MN 55905.

出版信息

Mayo Clin Proc. 1991 Dec;66(12):1209-16. doi: 10.1016/s0025-6196(12)62471-9.

Abstract

Type I anti-neuronal nuclear autoantibodies (ANNA-I, also known as "Hu") are a distinctive serologic marker of small cell lung carcinoma (SCLC) in patients who have peripheral neuropathies or encephalomyeloradiculopathies. A tumor antigen reactive with these antibodies has been identified by other investigators by Western blot analyses, but an antigen has not been localized in SCLC immunohistochemically. We therefore tested, by indirect immunofluorescence, the sera of 49 sequential ANNA-I-positive patients and 30 control subjects for IgG reactive with SCLC. Two tumor cell lines were tested, one established from the primary tumor of a patient with Lambert-Eaton syndrome and the second from the metastatic lesion of a patient without neurologic disease. IgG in all ANNA-I-positive sera bound to both tumors. In most instances, the pattern resembled that seen in neurons, with strong homogeneous nuclear staining, sparing of nucleoli, and faint cytoplasmic staining. A highly significant correlation was noted between endpoint dilutions obtained on SCLC substrates and on central and peripheral neurons (r = 0.863; P less than 0.001). IgG in 3 of 30 control sera bound in low titer to SCLC cells but not to neurons, and 9 control sera contained non-organ-specific anti-nuclear antibodies (ANA). The ANA IgG was absorbed equivalently by homogenates of SCLC or colonic adenocarcinoma cells. In contrast, the reactivity of ANNA-I IgG with cerebellar and myenteric plexus neurons was absorbed only by homogenized SCLC cells. These findings suggest that SCLC antigens account for all neuronal reactivity of ANNA-I. IgG of this specificity may serve as a useful reagent for identifying SCLC cells in surgical pathologic and cytologic specimens.

摘要

I型抗神经元核自身抗体(ANNA-I,也称为“Hu”)是患有周围神经病或脑脊髓神经根病的小细胞肺癌(SCLC)患者的一种独特血清学标志物。其他研究者通过蛋白质印迹分析鉴定出了一种与这些抗体反应的肿瘤抗原,但尚未通过免疫组织化学方法在SCLC中定位该抗原。因此,我们通过间接免疫荧光检测了49例连续的ANNA-I阳性患者和30例对照受试者血清中与SCLC反应的IgG。检测了两种肿瘤细胞系,一种是从患有兰伯特-伊顿综合征患者的原发性肿瘤建立的,另一种是从无神经系统疾病患者的转移病灶建立的。所有ANNA-I阳性血清中的IgG均与两种肿瘤结合。在大多数情况下,其模式类似于在神经元中看到的模式,核染色强烈均匀,核仁不着色,细胞质染色微弱。在SCLC底物以及中枢和周围神经元上获得的终点稀释度之间存在高度显著的相关性(r = 0.863;P < 0.001)。30例对照血清中有3例的IgG以低滴度与SCLC细胞结合,但不与神经元结合,9例对照血清含有非器官特异性抗核抗体(ANA)。ANA IgG被SCLC或结肠腺癌细胞匀浆等量吸收。相比之下,ANNA-I IgG与小脑和肌间神经丛神经元的反应性仅被匀化的SCLC细胞吸收。这些发现表明SCLC抗原解释了ANNA-I的所有神经元反应性。这种特异性的IgG可能是在手术病理和细胞学标本中鉴定SCLC细胞的有用试剂。

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