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首页> 外文期刊>Lung cancer: Journal of the International Association for the Study of Lung Cancer >Long acting somatostatin analogues in combination to antineoplastic agents in the treatment of small cell lung cancer patients
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Long acting somatostatin analogues in combination to antineoplastic agents in the treatment of small cell lung cancer patients

机译:长效生长抑素类似物联合抗肿瘤药治疗小细胞肺癌患者

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摘要

Background: Long acting somatostatin analogues combined with platinum analogues have demonstrated an antiproliferative effect on growth of human SCLC xenographs. Method: 130 previously untreated SCLC patients - 54 with limited disease (LD) and positive somatostatin receptors were included in the study. All patients performed 111In-Octreotide scanning before chemotherapy (CHT), every 3 months and up to 4 times. All patients were treated with paclitaxel 190mg/m 2+carboplatin AUC=5.5 for up to 6 cycles. 47/130 patients (Group A, control group) received only CHT. Forty eight hours after each CHT 43/130 patients (Group B) were also administered 30mg somatuline ? (lanreotide) by a single subcutaneous (s.c.) injection to stimulate somatostatin receptors (SSTRS) for 2 weeks. 40/130 patients (Group C) received 60mg somatuline ? autogel to stimulate SSTRS for 4 weeks. Patients in Groups A and B after the completion of the CHT continued maintenance therapy with somatuline. NSE, IGF1, VEGFA, VEGFC, VEGFR2, HER2 levels were monitored. In histological samples Bcl-2 and VEGF were also explored by immunohistochemistry. Results: No statistically significant differences were observed between the 3 Groups regarding LD and extensive disease (ED) patient ratios, age and PS. Group B had a survival benefit in comparison to Groups A and C (p=0.029). LD patients of Group B had a significant benefit compared to Groups A and C (p=0.012, Breslow test). In LD Group B had a significant longer TTP (p=0.02) in comparison to Groups A and C. Adverse effects had no statistically significant difference between the Groups and toxicity was well managed. Interpretation: Long acting somatostatin analogues could be used as an additive therapy in combination to antineoplastic agents in patients positive for somatostatin receptors. A dose of 30. mg improved survival only in LD SCLC patients.
机译:背景:长效生长抑素类似物与铂类似物结合已证明对人SCLC异位图的生长具有抗增殖作用。方法:130名先前未接受治疗的SCLC患者-54名患有有限疾病(LD)和生长抑素受体阳性的患者被纳入研究。所有患者每3个月进行一次111In-奥曲肽扫描(CHT),最多4次。所有患者均接受紫杉醇190mg / m 2 +卡铂AUC = 5.5的治疗,疗程长达6个周期。 47/130例患者(A组,对照组)仅接受CHT。每次CHT 43/130患者(B组)后四十八小时,也服用30mg Somatuline? (lanreotide)通过单次皮下(s.c.)注射刺激生长抑素受体(SSTRS)2周。 40/130名患者(C组)接受了60mg苦参碱?自动凝胶刺激SSTRS 4周。 CHT完成后,A组和B组的患者继续接受索马妥林维持治疗。监测NSE,IGF1,VEGFA,VEGFC,VEGFR2,HER2水平。在组织学样本中,还通过免疫组织化学探索了Bcl-2和VEGF。结果:3组之间在LD和广泛疾病(ED)患者的比率,年龄和PS方面未观察到统计学上的显着差异。与A组和C组相比,B组具有生存优势(p = 0.029)。与A组和C组相比,B组的LD患者具有显着获益(p = 0.012,Breslow检验)。与A和C组相比,LD B组的TTP显着更长(p = 0.02)。不良反应在各组之间没有统计学上的显着差异,并且毒性得到了很好的控制。解释:长生长抑素类似物可作为生长抑素受体阳性患者的抗肿瘤药联合使用。 30 mg剂量仅可改善LD SCLC患者的生存率。

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