Low-dose Imatinib Efficacy in a Gastrointestinal Stromal Tumor Patient With KIT Exon 11 W557_K558 Deletion.

IF 1.8 4区医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL

In vivo Pub Date : 2025-01-01 DOI:10.21873/invivo.13857

Hirotaka Suto, Miyuki Kawamura, Mitsunori Morita, Hideki Sakai, Takuma Onoe, Kyoko Ikeuchi, Kazuyoshi Kajimoto, Koji Matsumoto

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引用次数: 0

Abstract

Background/aim: Gastrointestinal stromal tumors (GISTs) are rare cancers originating from Cajal's stromal cells in the gastrointestinal tract. The most common driver mutation in these cancers is the KIT mutation. This report presents a case of response to low-dose imatinib in a patient with GIST harboring KIT exon 11 W557_K558 deletion.

Case report: In June 2023, an 82-year-old male developed perineal pain. Computed tomography (CT) imaging revealed a mass measuring >9 cm, extending from the rectum to the prostate. Submucosal tumor biopsy revealed a tumor with CD117-positive and DOG1-positive spindle-shaped cells leading to a diagnosis of GIST. c-Kit gene mutation analysis detected a W557_K558 deletion in exon 11. Treatment with imatinib (400 mg/day) was initiated in late October 2023 to preserve organ function; the dose was reduced to 300 mg/day after 5 days of treatment and further reduced to 200 mg/day after 10 days, with continued treatment at this dose. The CT performed in January, April, and June 2024 showed that the rectal GIST had shrunk. The blood imatinib concentration remained at approximately 650 ng/ml from January to March 2024 and decreased to 391 ng/ml in May 2024.

Conclusion: The response rate of GISTs to imatinib is influenced by genetic mutations. GIST with KIT exon 11 W557_K558 deletion is associated with a high risk of recurrence. In vitro data showed that low-dose imatinib was effective in such cases. Low-dose imatinib is a treatment option for patients with GIST harboring KIT exon 11 W557_K558 deletion who are intolerant to high-dose imatinib.

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低剂量伊马替尼对KIT外显子11 W557_K558缺失的胃肠道间质瘤患者的疗效

背景/目的：胃肠道间质瘤（gist）是一种起源于胃肠道Cajal间质细胞的罕见肿瘤。这些癌症中最常见的驱动突变是KIT突变。这篇报道提出了一例对低剂量伊马替尼有反应的GIST患者携带KIT外显子11 W557_K558缺失。病例报告：2023年6月，一名82岁男性出现会阴疼痛。计算机断层扫描（CT）成像显示肿块大小为bbb9cm，从直肠延伸到前列腺。粘膜下肿瘤活检显示cd117阳性和dog1阳性梭形细胞，诊断为GIST。c-Kit基因突变分析在第11外显子检测到W557_K558缺失。2023年10月下旬开始使用伊马替尼（400mg /天）治疗，以保持器官功能；治疗5天后剂量降至300 mg/天，10天后进一步降至200 mg/天，并继续以该剂量治疗。2024年1月、4月、6月CT示直肠GIST缩小。2024年1 - 3月血伊马替尼浓度维持在650 ng/ml左右，2024年5月降至391 ng/ml。结论：gist对伊马替尼的应答率受基因突变的影响。KIT外显子11 W557_K558缺失的GIST与高复发风险相关。体外实验数据显示，低剂量伊马替尼对此类病例有效。对于携带KIT外显子11 W557_K558缺失且对大剂量伊马替尼不耐受的GIST患者，低剂量伊马替尼是一种治疗选择。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

In vivo 医学-医学：研究与实验

CiteScore

4.20

自引率

4.30%

发文量

330

审稿时长

3-8 weeks

期刊介绍： IN VIVO is an international peer-reviewed journal designed to bring together original high quality works and reviews on experimental and clinical biomedical research within the frames of physiology, pathology and disease management. The topics of IN VIVO include: 1. Experimental development and application of new diagnostic and therapeutic procedures; 2. Pharmacological and toxicological evaluation of new drugs, drug combinations and drug delivery systems; 3. Clinical trials; 4. Development and characterization of models of biomedical research; 5. Cancer diagnosis and treatment; 6. Immunotherapy and vaccines; 7. Radiotherapy, Imaging; 8. Tissue engineering, Regenerative medicine; 9. Carcinogenesis.