Effects of PI3K Inhibitor NVP-BKM120 on Acquired Resistance to Gefitinib of Human Lung Adenocarcinoma H1975 Cells

The effects of class I PI3K inhibitor NVP-BKM120 on cell proliferation, cell cycle distri- bution, cellular apoptosis, phosphorylation of several proteins of the PI3K/AKT signaling pathway and the mRNA expression levels of HIFl-ct, VEGF and MMP9 in the acquired gefitinib resistant cell line H1975 were investigated, and whether NVP-BKM120 can overcome the acquired resistance caused by the EGFR T790M mutation and the underlying mechanism were explored. MTT assay was performed to detect the effect of gefitinib, NVP-BKM120, NVP-BKM120 plus 1 ~unol/L gefitinib on growth of H1975 cells. The distribution of cell cycle and apoptosis rate of H1975 cells were examined by using flow cytometry. The mRNA expression levels of tumor-related genes such as HIFI-a, VEGF and MMP9 were detected by using real-time quantitative PCR. Western blotting was used to detect the ex- pression level of phosphorylated proteins in the PI3K/AKT signaling pathway, such as Ser473-p-AKT, Ser235/236-p-S6 and Thr70-p-4E-BP1, as well as total AKT, $6 and 4E-BP1. The results showed that the NVP-BKM120 could inhibit the growth of H1975 cells in a concentration-dependent manner, and H1975 cells were more sensitive to NVP-BKM120 than gefitinib （IC50：1.385 vs. 15.09 ~mol/L respec- tively）, whereas combination of NVP-BKM120 and gefitinib （1 ~trnol/L） did not show more obvious ef- fect than NVP-BKM120 used alone on inhibition of cell growth （P〉0.05）. NVP-BKM120 （1 ~unol/L） increased the proportion ofH1975 cells in G0~G1 phase and the effect was concentration-dependent, and 2 ~maol/L NVP-BKM120 promoted apoptosis ofH1975 cells. There was no significant difference in the proportion of H1975 cells in G0-G1 phase and apoptosis rate between NVP-BKM120-treated alone group and NVP-BKM120 plus genfitinib （1 ~unol/L）-treated group or between DMSO-treated control group and gefitinib （1 Ixmol/L）-treated alone group （P〉0.05 for all）. It was also found that the mRNA expression levels of these genes were down-regulated by NVP-BKM120 （1 ~unol/L）, and NVP-BKM120 （1 ~tmol/L） or NVP-BKM120 （1 pmol/L） plus gefitinib （1 ~tmol/L） obviously inhibited the activation of Akt, $6 and 4E-BP1 as compared with control group, but single use of gefitinib （1 pmol/L） exerted no significant effect. These data suggested that NVP-BKM120 can overcome gefitinib resistance in H1975 cells, and the combination of NVP-BKM120 and gefitinib did not have additive or synergistic effects. It was also concluded that NVP-BKM120 could overcome the acquired resistance to gefitinib by down-regulating the phosphorylated protein in PI3K/AKT signal pathways in H1975 cells, but it could not enhance the sensitivity of H 1975 cells to gefitinib.

B细胞非霍奇金淋巴瘤靶向药物治疗研究进展

B细胞非霍奇金淋巴瘤(B-cell non-Hodgkin's lymphoma,B-NHLs)代表了一组异质性的来源于血液系统的恶性肿瘤,目前针对B-NHLs一线治疗方案仍是经典标准R-CHOP方案。近几年,靶向阻断分子或细胞机制在淋巴瘤中具有改变临床实践的意义,靶向治疗手段已成为了越来越重要的预测和肿瘤治疗方案,本文就近年来B-NHLs靶向治疗新进展作一综述。

患者自评类嗓音量表跨文化调适和信效度研究分析

患者自评类嗓音量表是量化嗓音问题严重程度及其对生活影响程度的重要工具,具有很高的临床价值。全球范围内有一系列患者自评类嗓音量表被广泛运用和跨语种推行,国内在患者自评类嗓音量表跨文化调适方面已有较多研究,不少临床常用量表已被汉化。然而,国内的相关研究主要针对个体量表进行,尚无对此类研究的综述,因此不易形成对患者自评类嗓音量表汉化情况的系统把握。本文对患者自评类嗓音量表汉化的质量、数量和类型进行了系统梳理,从宏观角度把握相关量表的跨文化调适和信效度检验现状,明确下一步研究工作的方向。

外周血效应型滤泡辅助性T细胞和滤泡辅助性T细胞亚型在系统性红斑狼疮发病机制中的作用

目的通过检测滤泡辅助性T细胞(Tfh)亚型及效应型滤泡辅助性T细胞(Tfhem)在系统性红斑狼疮(SLE)患者外周血中的表达情况,深入探讨它们作为SLE病情活动指标的血液标志物的价值。方法对象为2016年3月至2018年4月在北京大学人民医院风湿免疫科门诊或住院就诊的SLE患者64例及健康志愿者(正常对照)15名,应用流式细胞术检测SLE患者和正常对照者外周血中Tfh(CD3^+CD4^+CD45RA^-CXCR5^+)、细胞亚型Tfh1(CXCR3^+CCR6^-Tfh)、Tfh2(CXCR3-CCR6^+Tfh)、Tfh17(CXCR3-CCR6^+Tfh)和Tfhem(CCR7^lowPD-1^highTfh)的表达。收集入组的SLE患者的临床资料及实验室检查指标,分析Tfh细胞亚型、Tfhem细胞与实验室指标、SLE疾病活动度和不同临床表型的相关性。结果SLE患者外周血中Tfhem细胞的表达率明显高于正常对照组(1.40±1.12比0.51±0.24,P<0.0001),Tfhem细胞的表达与SLE病情活动度(SLEDAI)(P=0.0153)、抗双链DNA抗体(anti-dsDNAantibody)(P=0.0031)有显著相关性,与补体C3,补体C4,红细胞沉降率(ESR),C反应蛋白(CRP)无明显相关性。Tfh2的表达率明显高于正常对照组(3.83±2.74比2.18±1.07,P=0.0004),而Tfh1和Tfh17在两组中表达无明显差异,抗dsDNA抗体高的患者的Tfh2表达高于抗dsDNA抗体低的患者,但差异无统计学意义(4.33±3.20比3.70±1.070,P=0.0696)。结论Tfhem的表达与SLE的病情活动有关,有可能作为SLE病情进展及治疗效果的评价指标,Tfhem的表达同时与抗dsDNA抗体相关,因此,它在SLE发病过程抗体的生成中发挥着重要作用,甚至可能成为治疗SLE的靶细胞;Tfh2在SLE患者外周血中明显升高,与抗dsDNA抗体有一定的相关性,可能参与了SLE的病情进展。