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Precision treatment in colorectal cancer: Now and the future

机译:大肠癌的精准治疗:现在和将来

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Until recently, a one‐drug‐fits‐all model was applied to every patient diagnosed with the same condition. But not every condition is the same, and this has led to many cases of ineffective treatment. Pharmacogenetics is increasingly used to stratify patients for precision medicine treatments, for instance, the UGT1A1*28 polymorphism as a dosage indicator for the use of irinotecan as well as epidermal growth factor receptor (EGFR) immunohistochemistry and KRAS Proto‐Oncogene ( KRAS ) exon 2 mutation tests for determining the likelihood of treatment response to cetuximab or panitumumab treatment in metastatic colorectal cancer (CRC). The other molecular subtypes, such as KRAS exon 3/4, B‐Raf Proto‐Oncogene, NRAF , PIK3CA , and PETN , were also reported as potential new pharmacogenetic targets for the current and the newly discovered anticancer drugs. In addition to next‐generation sequencing (NGS), primary tumor cells for in vivo and in vitro drug screening, imaging biomarker 3′‐Deoxy‐3′‐18F‐fluorothymidine positron emission tomography, and circulating tumor DNA (ctDNA) detection methods are being developed and may represent the future direction of precision medicine. This review will discuss the current environment of precision medicine, including clinically approved targeted therapies, the latest potential therapeutic agents, and the ongoing pharmacogenetic trials for CRC patients.
机译:直到最近,对所有被诊断出患有相同疾病的患者都采用了一种“一药多用”的模型。但是,并非每种情况都是一样的,这导致许多无效的治疗案例。药物遗传学已越来越多地用于对患者进行精确药物治疗的分层,例如,UGT1A1 * 28多态性作为使用伊立替康以及表皮生长因子受体(EGFR)免疫组化和KRAS原癌基因(KRAS)外显子2的剂量指标突变测试,用于确定转移性结直肠癌(CRC)对西妥昔单抗或帕尼单抗治疗的反应可能性。其他分子亚型,例如KRAS外显子3/4,B-Raf原癌基因,NRAF,PIK3CA和PETN也被报道为当前和新发现的抗癌药物的潜在新药理学靶标。除下一代测序(NGS)之外,还有用于体内和体外药物筛选的原发性肿瘤细胞,生物标志物3'-Deoxy-3'-18F-氟胸苷正电子发射断层显像成像以及循环肿瘤DNA(ctDNA)检测方法。的发展,可能代表精密医学的未来方向。这篇综述将讨论精确医学的当前环境,包括临床批准的靶向疗法,最新的潜在治疗剂以及正在进行的针对CRC患者的药物遗传学试验。

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