SP174,NRAS Q61R突变特异性抗体,在结直肠癌中与KRAS Q61R突变蛋白发生交叉反应。
SP174, NRAS Q61R Mutant-Specific Antibody, Cross-Reacts With KRAS Q61R Mutant Protein in Colorectal Carcinoma.
作者信息
Lasota Jerzy, Kowalik Artur, Felisiak-Golabek Anna, Inaguma Shingo, Wang Zeng-Feng, Pięciak Liliana, Zięba Sebastian, Pęksa Rafał, Kopczynski Janusz, Okoń Krzysztof, Waloszczyk Piotr, Gozdz Stanislaw, Biernat Wojciech, Miettinen Markku
机构信息
From the Laboratory of Pathology, National Cancer Institute, Bethesda, Maryland (Drs Lasota, Felisiak-Golabek, Inaguma, Wang, and Miettinen); the Departments of Molecular Diagnostics (Dr Kowalik, Ms Pięciak, and Mr Zięba), Surgical Pathology (Dr Kopczynski), and Clinical Oncology (Dr Gozdz), Holycross Cancer Center, Kielce, Poland; the Department of Pathology, Aichi Medical University School of Medicine, Nagakute, Japan (Dr Inaguma); the Department of Pathomorphology, Medical University of Gdansk, Poland (Drs Pęksa and Biernat); the Department of Pathomorphology, Jagiellonian University, Krakow, Poland (Dr Okoń); ZDUNOMED/Histopathology, Szczecin, Poland (Dr Waloszczyk); and Faculty of Health Sciences, The Jan Kochanowski University, Kielce, Poland (Dr Gozdz). Drs Lasota and Kowalik contributed equally to this work.
出版信息
Arch Pathol Lab Med. 2017 Apr;141(4):564-568. doi: 10.5858/arpa.2016-0147-OA. Epub 2017 Feb 28.
Abstract
CONTEXT
- NRAS is a member of the RAS family oncoproteins implicated in cancer. Gain-of-function NRAS mutations were reported in a subset of colorectal cancers. These mutations occur at codons 12, 13, and 61 and are detected by molecular genetic testing. Recently, an antibody (clone SP174) became available to immunohistochemically pinpoint NRAS Q61R mutant protein. In malignant melanoma, NRAS Q61R mutant-specific immunohistochemistry was shown to be a valuable supplement to traditional genetic testing.
OBJECTIVE
- To evaluate the significance of NRAS Q61R mutant-specific immunohistochemistry in a cohort of colorectal carcinomas.
DESIGN
- A total of 1185 colorectal carcinomas were immunohistochemically evaluated with SP174 antibody. NRAS Q61R mutant-specific immunohistochemistry was validated by molecular genetic testing including Sanger sequencing, quantitative polymerase chain reaction (qPCR), and next-generation sequencing.
RESULTS
- Twelve tumors showed strong SP174 immunoreactivity. Sanger sequencing detected an identical c.182A>G substitution, causing NRAS Q61R mutation at the protein level, only in 8 SP174-positive cases. These results were confirmed by qPCR study. Subsequently, NRAS wild-type tumors with strong SP174 staining were evaluated by next-generation sequencing and revealed KRAS c.182A>G substitutions predicted to cause KRAS Q61R mutation. Review of colorectal carcinomas with known KRAS and NRAS genotype revealed that none of 62 wild-type tumors or 47 mutants other than Q61R were SP174 positive.
CONCLUSION
- SP174 immunohistochemistry allows sensitive detection of NRAS and KRAS Q61R mutants. However, molecular genetic testing is necessary to determine specifically which RAS gene is mutated.
摘要
背景
NRAS是与癌症相关的RAS家族癌蛋白成员。在一部分结直肠癌中报道了功能获得性NRAS突变。这些突变发生在密码子12、13和61位,可通过分子遗传学检测发现。最近,一种抗体(克隆号SP174)可用于免疫组织化学定位NRAS Q61R突变蛋白。在恶性黑色素瘤中,NRAS Q61R突变特异性免疫组织化学被证明是传统基因检测的有价值补充。
目的
评估NRAS Q61R突变特异性免疫组织化学在一组结直肠癌中的意义。
设计
用SP174抗体对总共1185例结直肠癌进行免疫组织化学评估。NRAS Q61R突变特异性免疫组织化学通过包括桑格测序、定量聚合酶链反应(qPCR)和下一代测序在内的分子遗传学检测进行验证。
结果
12例肿瘤显示出强烈的SP174免疫反应性。桑格测序仅在8例SP174阳性病例中检测到相同的c.182A>G替代,导致蛋白质水平的NRAS Q61R突变。qPCR研究证实了这些结果。随后,对具有强烈SP174染色的NRAS野生型肿瘤进行下一代测序,发现KRAS c.182A>G替代,预计会导致KRAS Q61R突变。对已知KRAS和NRAS基因型的结直肠癌进行回顾发现,62例野生型肿瘤或除Q61R之外的47例突变体中均无SP174阳性。
结论
SP174免疫组织化学可敏感检测NRAS和KRAS Q61R突变体。然而,需要分子遗传学检测来具体确定哪个RAS基因发生了突变。
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