KRAS和her家族基因在壶腹癌中的突变特征

Q3 Medicine

中华病理学杂志 Pub Date : 2025-07-08 DOI:10.3760/cma.j.cn112151-20250326-00210

L L Zeng, S F Wu, W X Zhou, Y Y Liu, K M Li, S W Mo, M L Liu, X Zeng

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Results: In our cohort (22 males, 15 females; 31-82 years old), KRAS gene mutations were detected in 51.4% (19/37) of cases, with G12D being the most frequent abnormality (7/19), followed by G12V (5/19) and Q61R (3/19). Other variants of KRAS gene included G12C, A146T, N116H, and Q61H (each 1/19). In this cohort, 27.0% (10/37) of cases harbored HER-family gene alterations with most frequently in HER2 (6/10) and HER3 genes (missense mutations mainly). Notably, 3 cases (8.1%, 3/37) with coexistence of KRAS and HER-family genes mutations were recognized in our series, including KRAS p.G12D/HER2 p.V842I/HER2 p.V777L (c.2329 G>T)/HER3 p.Asp581Asn, KRAS p.Q61R/HER4 p.D1018H and KRAS p.G12C/HER2 p.R678Q. Additionally, a mutation of HER3 p.V104L (c.310 G>C) was identified in our population. Moreover, 4 novel mutations including HER3 p.V296E, HER3 p.V920L (c.2758 G>T), HER3 p.Asp581Asn, and HER4 p.D1018H were detected. In 6 tumors with HER2 gene changes (16.2%, 6/37), 5 variants with the high proportion of HER2 p.S310Y (3/6) were revealed. A tumor (HER2 IHC 2+) with HER2 p.S310Y presented HER2 gene amplification confirmed by NGS and FISH, and another one (also HER2 IHC 2+) with HER2 p.L755S possessed HER2 gene amplification determined by FISH assay. 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引用次数: 0

摘要

目的：探讨KRAS和her家族基因在壶腹癌患者中的变异及共变情况。方法：采用新一代测序技术（NGS）对2019年4月至2024年10月北京联合医院采集的37例经福尔马林固定石蜡包埋的原发性壶腹癌标本进行KRAS和her家族基因突变分析。免疫组织化学（IHC）检测HER2突变病例的HER2蛋白表达，荧光原位杂交（FISH）检测HER2 IHC 2+病例的基因状态。结果：在我们的队列中(22名男性，15名女性；31 ~ 82岁)，KRAS基因突变占51.4%(19/37)，其中以G12D最为常见（7/19），其次为G12V（5/19）和Q61R（3/19）。KRAS基因的其他变异包括G12C、A146T、N116H和Q61H（各为1/19）。在该队列中，27.0%（10/37）的病例携带her家族基因改变，最常见的是HER2（6/10）和HER3基因（主要是错义突变）。值得注意的是，在我们的系列中发现了3例（8.1%,3/37）KRAS和her家族基因共存突变，包括KRAS p.G12D/HER2 p.V842I/HER2 p.V777L （c.2329）G>T)/HER3 p.Asp581Asn, KRAS p.Q61R/HER4 p.D1018H和KRAS p.G12C/HER2 p.R678Q。此外，HER3 p.V104L基因突变(c.310在我们的人群中发现了G b> C)。此外，HER3 p.V296E、HER3 p.V920L (c.2758检测到G>T)、HER3 p.Asp581Asn、HER4 p.D1018H。在6例HER2基因改变的肿瘤中（16.2%,6/37），发现HER2 p.S310Y高比例的变异5例（3/6）。一个HER2 p.S310Y的肿瘤（HER2 IHC 2+）经NGS和FISH证实有HER2基因扩增，另一个HER2 p.L755S的肿瘤（HER2 IHC 2+）经FISH检测有HER2基因扩增。结论：壶腹癌中存在KRAS与her -家族基因共变，HER2基因突变占her -家族基因异常的一半以上，且可能伴有基因扩增。

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[Characteristics of KRAS and HER-family gene mutations in ampullary cancer].

Objective: To investigate the variations and co-alteration of KRAS and HER-family genes in the patients with ampullary carcinoma. Methods: A total of 37 formalin-fixed paraffin-embedded primary ampullary carcinoma specimens, which were collected at Peking Union Medical College Hospital from April 2019 to October 2024 were analyzed for KRAS and HER-family gene mutations using next-generation sequencing (NGS). Immunohistochemistry (IHC) was performed for HER2 protein expression in HER2 mutation cases and fluorescence in situ hybridization (FISH) for further gene status in HER2 IHC 2+cases. Results: In our cohort (22 males, 15 females; 31-82 years old), KRAS gene mutations were detected in 51.4% (19/37) of cases, with G12D being the most frequent abnormality (7/19), followed by G12V (5/19) and Q61R (3/19). Other variants of KRAS gene included G12C, A146T, N116H, and Q61H (each 1/19). In this cohort, 27.0% (10/37) of cases harbored HER-family gene alterations with most frequently in HER2 (6/10) and HER3 genes (missense mutations mainly). Notably, 3 cases (8.1%, 3/37) with coexistence of KRAS and HER-family genes mutations were recognized in our series, including KRAS p.G12D/HER2 p.V842I/HER2 p.V777L (c.2329 G>T)/HER3 p.Asp581Asn, KRAS p.Q61R/HER4 p.D1018H and KRAS p.G12C/HER2 p.R678Q. Additionally, a mutation of HER3 p.V104L (c.310 G>C) was identified in our population. Moreover, 4 novel mutations including HER3 p.V296E, HER3 p.V920L (c.2758 G>T), HER3 p.Asp581Asn, and HER4 p.D1018H were detected. In 6 tumors with HER2 gene changes (16.2%, 6/37), 5 variants with the high proportion of HER2 p.S310Y (3/6) were revealed. A tumor (HER2 IHC 2+) with HER2 p.S310Y presented HER2 gene amplification confirmed by NGS and FISH, and another one (also HER2 IHC 2+) with HER2 p.L755S possessed HER2 gene amplification determined by FISH assay. Conclusion: In ampullary carcinoma, co-alteration of KRAS and HER-family genes is observed, and HER2 gene mutations account for more than half of HER-family gene abnormities, which may be accompanied by gene amplification.

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中华病理学杂志 Medicine-Medicine (all)

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1.00

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0.00%

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10377

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