Navigating Ongoing Challenges in GI Stromal Tumors.

Q1 Medicine

American Society of Clinical Oncology educational book / ASCO. American Society of Clinical Oncology. Meeting Pub Date : 2025-06-01 Epub Date: 2025-05-20 DOI:10.1200/EDBK-25-473224

Heikki Joensuu, Hirotaka Miyashita, Suzanne George, Jason Sicklick

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Abstract

GI stromal tumors (GISTs) are mesenchymal neoplasms with variable natural histories, originating in the GI tract, most commonly in the stomach. They are frequently characterized by KIT or platelet-derived growth factor receptor alpha (PDGFRA) oncogenic mutations. Surgical resection remains the cornerstone treatment for localized GISTs. Clinical trials have demonstrated the benefits of adjuvant imatinib in patients selected on the basis of recurrence risk and gene mutations, although the optimal duration of therapy is yet to be established. Some data suggest that longer durations of adjuvant imatinib (>3 years) may provide additional benefit, which is being investigated in ongoing trials. Management of imatinib-related adverse effects is essential during treatment, and longitudinal abdominal imaging is mandatory both during and after adjuvant therapy. Once GISTs are more advanced and unresectable, KIT- and PDGFRA-directed tyrosine kinase inhibitors (TKIs) become the key treatment in most patients with KIT mutation. Several TKIs have regulatory approval for advanced GISTs, but in most patients, resistance to TKIs eventually emerges, mainly from secondary resistance mutations in KIT. Each TKI has different coverage of oncogenic KIT mutations, suggested by preclinical and clinical findings, which has given rationale to an ongoing clinical trial that includes molecular selection as eligibility criteria. Furthermore, novel treatment approaches, from TKI combinations to an antibody-drug conjugate, are being investigated. Despite the significant advance in managing GISTs with KIT mutations, those without KIT or PDGFRA mutation, which consists of 10%-15% of patients with GIST, can be a clinical challenge in the advanced setting. These non-KIT/PDGFRA GISTs could be driven by genomic or epigenomic alterations in SDHx, NF1 mutations, and other genomic alterations. Non-KIT/PDGFRA GISTs are less responsive to currently available TKIs than GISTs driven by KIT/PDGFRA mutations, and each subset of non-KIT/PDGFRA GIST has distinctive biology and clinical features. Therefore, individualized, multidisciplinary, biology-based management and consideration for clinical trial enrollment are critical for non-KIT/PDGRFA GISTs.

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胃肠道间质肿瘤的持续挑战。

胃肠道间质瘤（gist）是一种具有不同自然历史的间质肿瘤，起源于胃肠道，最常见于胃。它们通常以KIT或血小板衍生生长因子受体α (PDGFRA)致癌突变为特征。手术切除仍然是局部gist的基础治疗方法。临床试验已经证明，在根据复发风险和基因突变选择的患者中，辅助伊马替尼的益处，尽管最佳治疗持续时间尚未确定。一些数据表明，更长时间的伊马替尼辅助治疗（大约3年）可能会提供额外的益处，目前正在进行的试验中对此进行研究。治疗过程中伊马替尼相关不良反应的管理是必不可少的，在辅助治疗期间和之后都必须进行纵向腹部成像。一旦gist进展到晚期且无法切除，KIT和pdgfr导向的酪氨酸激酶抑制剂（TKIs）就成为大多数KIT突变患者的关键治疗方法。一些TKIs已获得晚期gist的监管批准，但在大多数患者中，最终会出现对TKIs的耐药性，主要来自KIT的继发性耐药突变。根据临床前和临床研究结果，每种TKI都有不同的致癌KIT突变覆盖范围，这为正在进行的包括分子选择作为资格标准的临床试验提供了理由。此外，新的治疗方法，从TKI联合到抗体-药物偶联，正在研究中。尽管在处理KIT突变的GIST方面取得了重大进展，但那些没有KIT或PDGFRA突变的患者（占GIST患者的10%-15%）在晚期可能是一个临床挑战。这些非kit /PDGFRA gist可能由SDHx、NF1突变和其他基因组改变的基因组或表观基因组改变驱动。与KIT/PDGFRA突变驱动的GIST相比，非KIT/PDGFRA GIST对当前可用TKIs的反应较差，并且非KIT/PDGFRA GIST的每个子集具有独特的生物学和临床特征。因此，个性化、多学科、基于生物学的管理和临床试验入组的考虑对于非kit /PDGRFA gist至关重要。

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

American Society of Clinical Oncology educational book / ASCO. American Society of Clinical Oncology. Meeting Medicine-Medicine (all)

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期刊介绍： The Ed Book is a National Library of Medicine–indexed collection of articles written by ASCO Annual Meeting faculty and invited leaders in oncology. Ed Book was launched in 1985 to highlight standards of care and inspire future therapeutic possibilities in oncology. Published annually, each volume highlights the most compelling research and developments across the multidisciplinary fields of oncology and serves as an enduring scholarly resource for all members of the cancer care team long after the Meeting concludes. These articles address issues in the following areas, among others: Immuno-oncology, Surgical, radiation, and medical oncology, Clinical informatics and quality of care, Global health, Survivorship.