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Lung adenocarcinoma organoids harboring EGFR 19Del and L643V double mutations respond to osimertinib and gefitinib

机译:肺腺癌有机体含EGFR 19DEL和L643V双突变对Osimertinib和Gefitinib的反应

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INTRODUCTION:It has been well reported that non-small-cell lung cancer (NSCLC) patients with single epithelial growth factor receptor (EGFR) activating mutation have high objective response rate when treated with EGFR-TKIs. However, due to rarity of cases, the response of patients with EGFR double or multiple mutations is not yet well understood. Patient-derived organoid technology has become to a powerful tool in cancer personalized medicine.PATIENT CONCERNS:A 60-year-old nonsmoking female was admitted to hospital for lung cancer after Chest CT.DIAGNOSES:The patient had no obvious clinical symptoms. Postoperative pathology confirmed a stage I of NSCLC. An EGFR double mutation 19Del/L643V was detected in the sequence of patient's cancer specimen.INTERVENTIONS:The patient was in good condition after surgical resection, with no sign of lung cancer recurrence. The patient has not yet started on targeted medicine.OUTCOMES:A lung cancer organoid culture was established from the cancer tissue of the patient, which recapitulated the morphological and molecular characteristics of cancer tissue. The drug sensitivity test showed that the cancer organoids that retained original mutations were sensitive to anticancer agents osimertinib and gefitinib, while resistant to erlotinib and icotinib.CONCLUSION:The uncommon EGFR double mutation exhibits distinctive sensitivities towards different target drugs of EGFR-TKIs. Our findings provide a better understanding of EGFR-TKIs' effects on patient-derived cancer organoids harboring uncommon EGFR double mutation(s).Copyright ? 2021 the Author(s). Published by Wolters Kluwer Health, Inc.
机译:介绍:已经良好地报道,当用EGFR-TKIS处理时,具有单个上皮生长因子受体(EGFR)激活突变的非小细胞肺癌(NSCLC)患者具有高的客观反应速率。然而,由于罕见的情况,EGFR双或多个突变患者的响应尚不清楚。患者衍生的有机体技术已成为癌症个性化医学的强大工具。胸部CT.diagnoses后,一名60岁的Nonsmoking女性被入住于肺癌中的医院:患者没有明显的临床症状。术后病理学确认了NSCLC的阶段。在患者癌症样本序列中检测到EGFR双突变19del / L643V.Interventions:患者在手术切除后处于良好状态,没有肺癌复发的迹象。患者尚未开始有针对性的药物。从患者的癌症组织建立了肺癌有机体培养物,该组织综合癌组织的形态学和分子特征。药物敏感性试验表明,保留了原始突变的癌细胞对抗癌剂Osimertinib和Gefitinib敏感,同时抵抗Erlotinib和icotinib。结论:罕见的EGFR双突变对EGFR-TKIS的不同靶药物表现出独特的敏感性。我们的研究结果提供了更好地理解EGFR-TKIS对患者衍生的癌细胞软件含有罕见的EGFR双突变的患者衍生的癌细胞体.Copyright? 2021提交人。由Wolters Kluwer Health,Inc。出版

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