CircTHSD4 promotes the malignancy and docetaxel (DTX) resistance in prostate cancer by regulating miR-203/HMGA2 axis

Objective:Circular ribose nudeic acids(circRNAs)are implicated in tumor progression and drug resistance of prostate cancer(PCa).The current work explored the function of circ_0005203(aircTHSD4)in the malignancy and docetaxel(DTX)resistance of PCa.Methods:circTHSD4 expression within PCa as well as matched non-carcinoma samples was measured through real time reverse transcription quantitative polymerase chain reaction(RT-qPCR).In addition,a subcellular fraction assay was conducted to determine circTHSD4 subcellular localization within PCa cells.In addition,we performed a Western blot(WB)assay to detect high mobility.group A2 protein(HMGA2)levels.Besides,functional associations of two molecules were investigated through dual luciferase reporter assay.Cell Counting Kit(CCK)-8,colony formation together with Transwell assay was conducted to assess malignant phenotypes of PCa cells,whereas flow cytometry was performed to determine cell apoptosis.Furthermore,a xenograft mouse model was constructed to verify the effect of circTHSD4 on the carcinogenesis of PCa cells.Results:According to RT-qPCR results,circTHSD4 was up-regulated within PCa tissues and cells,which predicted the dismal prognostic outcome of PCa cases.circTHSD4 silencing within PCa cells markedly suppressed cell growth,migration,and colony fomation.circTHSD4 silencing remarkably elevated PCa cell apoptosis and carcinogenesis within the xenograft model.Further,circTHSD4 silencing enhanced docetaxel(DTX)sensitivity in PCa cells.Furthermore,we demonstrated that circTHSD4 modulated the malignancy of PCa cells by regulating HMGA2 expression through sponging miR 203.Conclusion:Together,our findings suggest that cirCTHSD4 overexpression could promote the malignant phenotype and DTX resistance in PCa through the regulation of the miR 203/HMGA2 axis.

Development and Validation of a UPLC Method for the Determination of Docetaxel and Its Related Substances in Pharmaceutical Dosage Forms, an Antineoplastic Agent

A novel, simple, and sensitive Ultra Performance Liquid Chromatography (UPLC) method was developed and validated for the quantification of process-related impurities and degradants, as well as the assay of Docetaxel. The stability-indicating capability of the method was demonstrated through forced degradation studies and a comprehensive mass balance evaluation. Chromatographic separation was achieved using an ACQUITY UPLC BEH C18 column (100 × 2.1 mm, 1.7 µm), with gradient elution. The mobile phase A comprised a mixture of water, methanol, and acetonitrile (500:300:200, v/v/v), while mobile phase B was acetonitrile and water (800:200, v/v). The flow rate was set at 0.4 mL/min, with detection at 232 nm using a photodiode array detector. The method exhibited excellent performance, with a tailing factor of 1.10 for Docetaxel. The method was rigorously validated for precision, accuracy, linearity, LOD, LOQ, ruggedness, specificity, and robustness. Forced degradation studies confirmed the method’s suitability for stability analysis. Stability testing on the drug substance was conducted following ICH guidelines.

Acute severe hypokalemia caused by treatment of tongue squamous cell carcinoma with docetaxel and cisplatin:A case report

BACKGROUND The tongue squamous cell carcinoma(TSCC)is an oral malignant tumor arising from the squamous epithelium of the tongue mucosa,characterized by a high malignant degree,invasive growth,early lymph node metastasis,and poor prognosis.Paclitaxel,represented by docetaxel,is now the standard first-line treatment for head and neck squamous cell carcinoma.Docetaxel,which belongs to the class of drugs known as paclitaxel,is an antitumor drug that inhibits cell mitosis and proliferation.Its adverse effects include myelosuppression,hair loss,gastrointestinal reactions,fluid retention,and allergic reactions.However,hypokalemia is rare,most cases are mild or moderate,and severe hypokalemia is seldom reported.symptoms of adverse effects early.It is necessary to be considerate regarding individual differences between patients when selecting chemotherapy regimens and adhere to the principle of individualized treatment.Following multiple cycles of chemotherapy,patients should be aware of the accumulation of toxic side effects and receive blood tests reviewed within 24 hours of completion.It is essential to monitor electrolyte levels in patients suffering from severe gastrointestinal reactions to avoid complications that may result in death.

基于Doc2vec-LightGBM的CBTC车载信号设备故障分类诊断方法

车载信号设备是城市轨道交通信号系统的重要组成部分,其运营过程中会产生海量离散化、片段化的日志文本数据。目前,CBTC车载设备故障记录文本仍存在语义不明确、词语冗余的问题,从而造成故障致因溯源难,针对此,提出一种基于Doc2vec-LightGBM的CBTC车载设备故障自动分类诊断方法。首先对故障文本使用Jieba完成文本分词,依据TF-IDF实现分词文本数据的特征提取,并采用Doc2vec训练文本分词向量;其次针对数据不均衡的问题,采用Borderline-SMOTE算法进行少数类文本向量数据的补全泛化;最后,通过训练轻量梯度提升机LightGBM分类器完成故障文本自动分类。采用某信号厂商所记录的1 133条故障文本数据进行分类实验分析,并与支持向量机(SVM)方法对比。实验结果表明,所提方法在分类精确率、召回率上分别为98.2%、97.5%,证明了该故障文本自动分类方法的有效性和优越性。

车用柴油机DOC应对不同细分市场的开发

中国车用柴油机已执行国六排放标准,需要使用柴油机氧化催化器(DOC)才能满足法规要求。本文以某款重型柴油机为基础,搭载多通道排放测试发动机台架,对比不同方案DOC对一氧化氮(NO)转化效率、碳氢(HC)起燃、选择性催化还原(SCR)转化效率等影响,得出DOC配方变化对催化器性能影响的规律。结合车用柴油机在不同细分市场的使用需求,给出满足车辆应用及成本最优的差异化DOC方案。

环境温度对DOC前温度合理性故障影响性分析

选取一辆满足国六排放标准的重型柴油车,在高温、常温、低温环境开展实际道路整车后处理DOC前温度合理性故障验证。结果表明:在不同环境温度下,DOC前温度合理性故障均能满足监控条件,能够正常报出故障且无误报,满足开发及法规要求。高温环境故障报出时间在240s,常温和低温环境故障报出时间在300s。DOC前温度合理性故障在不同环境故障报出工况基本一致,发动机转速在(1400~2000)rpm,车速在(60~80)km/h。这个测试结果对下阶段法规整车OBD后处理合理性故障检测方法提供依据,减少故障在实际道路的检测时间。

DOC+DPF对防爆柴油机气态污染物影响的试验研究

非道路柴油机国四排放标准HJ1014-2020《非道路柴油移动机械污染物排放控制技术要求》要求在2022年12月1日起非道路移动机械用柴油机必须满足国四排放要求,矿用防爆柴油机为满足国四排放要求也要做充足的前期研究。非道路柴油机多采用DOC+DPF的路线使得CO和颗粒满足国四排放要求,防爆柴油机的CO和颗粒实现国四排放要求也可以通过使用DOC+DPF达到。MT990要求防爆柴油机的表面温度不能超过150℃,使得DOC和DPF也需进行防爆改装后才能使用,所以增加防爆改装后的DOC+DPF对防爆柴油机的尾气排放究竟有何影响还有待实验验证。本文通过防爆柴油机台架试验研究防爆改装后的DOC+DPF对防爆柴油机排放的影响。

DOC及POC对柴油机污染物NOx和PM的影响

柴油机的不断发展也给人类和地球环境带来了日益严重的污染问题。为了满足日益严苛的排放法规和更高的性能要求,本文重点通过ESC试验循环和稳态满载试验,研究不同的氧化催化器及颗粒物催化氧化器组合对柴油机污染物中的NOx和PM的影响。

DOC和金属DPF对柴油机排气中碳烟纳观结构特性的影响

开展了柴油机氧化催化器(DOC)和金属DPF对柴油机排气中碳烟纳观结构特性的影响研究。结果表明:原机排气中碳烟平均微晶长度(L_(p))随负荷的增加而增大,随转速的升高而减小;平均微晶层间距(D_(p))和平均微晶曲率(T_(p))的变化规律与L_(p)相反。经过DOC处理后,L_(p)增大,D_(p)和T_(p)减小;而它们的变化幅度均随负荷的增大而增大,随转速的升高而减小。金属DPF对碳烟3个纳观结构特性参数的影响均不大。原机排气中碳烟的L_(p)、D_(p)和T_(p)均与碳烟氧化反应表观活化能(E_(a))具有密切的相关性,其中,T_(p)与E_(a)的决定系数最大;经过DOC处理后,L_(p)、D_(p)和T_(p)与E_(a)的决定系数均略有增加。

Survivin反义核酸诱导卵巢癌细胞SKOV3凋亡及对docetaxel的增敏作用

背景与目的:Survivin在大多数肿瘤组织中特异性高表达,并与肿瘤细胞的凋亡和耐药密切相关。本研究探讨Survivin反义真核表达载体(anti-pcDNA3-svv)对卵巢癌细胞SKOV3凋亡的诱导作用及对docetaxel的增敏作用。方法:采用Survivin反义核酸瞬时电转染法转染SKOV3细胞,筛选出阳性细胞株。以RT-PCR检测survivinmRNA的表达,Westernblot检测Survivin蛋白的表达。用流式细胞仪和透射电镜观察Survivin反义核酸对SKOV3细胞凋亡的诱导作用,MTT法检测其对docetaxel的增敏作用。结果:稳定表达anti-pcDNA3-svv的SKOV3细胞survivinmRNA及Survivin蛋白均比未转染者明显降低,透射电镜下可见稳定转染组细胞呈凋亡晚期变化,流式细胞仪显示其凋亡率为19%,docetaxel对实验组细胞的IC50值为(13.3±2.2)ng/ml,而对照组为(53.2±2.4)ng/ml,差异具有显著性(P<0.05)。结论:Survivin反义核酸可诱导SKOV3细胞凋亡,增强SKOV3细胞对docetaxel的敏感性。

Docetaxel对涎腺粘液表皮样癌高转移细胞增殖及转移力的抑制作用

目的 :研究Docetaxel对涎腺粘液表皮样癌高转移细胞M3 SP4 增殖及转移力的抑制作用。方法 :用细胞计数法、克隆形成法、流式细胞术、癌细胞裸鼠尾静脉注射法、癌细胞裸鼠颌下腺原位接种法研究Docetaxel对M3 SP4 细胞增殖及转移力的抑制作用。结果 :Docetaxel对M3 SP4 细胞具有浓度及时间依赖性生长抑制作用 ,作用 72h后 ,IC3 0 和IC50 分别为 0 .34nmol/L和 0 .6 3nmol/L ;IC3 0 浓度的药物作用于M3 SP4 细胞 ,对照组及处理组细胞群体倍增时间分别为 32 .7h和 43h ;对照组及药物作用浓度分别为 0 .0 5nmol/L及 0 .1nmol/L时 ,克隆形成率为 ( 2 9.2± 1.4) %和 ( 2 0 .2± 0 .8) % ,( 2 .8± 0 .4) % ;在裸鼠体内实验中对照组及治疗组〔30mg/(kg·周 )〕肺表面的转移结节数为 11± 3.4和 0 ;裸鼠颌下腺重量 ( g)为 1.2 0± 0 .2 3和 0 .31±0 .0 5。结论 :Docetaxel可明显抑制M3 SP4 细胞的增殖及转移力。

再放疗并同步使用Docetaxel在鼻咽癌放疗后复发病人中的应用

目的:不能手术切除的鼻咽癌放疗后再复发的病人,其治疗困难,化疗疗效差,而单独再放疗只能挽救一小部分病人,本文探讨再放疗并同步使用多西紫彬醇(Docetaxel)在鼻咽癌首次放疗后复发病人中可行性及毒副反应,并评价其疗效。方法:对11例鼻咽癌足量放疗后经组织病理学证实复发、而无法行手术及腔内放疗的患者进行了同步放化疗。放疗采用三维适形放疗,外照射鼻咽部,分次量为1.8Gy,总剂量为36Gy-39.6Gy。化疗采用Docetaxel,15mg/m2,每周一次,静脉滴注。结果:10%、33%的患者分别出现Ⅲ度、Ⅳ度皮肤反应,18%、10%的病人分别出现Ⅲ度、Ⅳ度黏膜反应,18%患者出现Ⅲ度恶心呕吐,27%的患者出现Ⅲ度-Ⅳ度白细胞下降,10%患者出现Ⅲ度血小板下降。1例患者因严重的黏膜反应致使治疗延迟2周。治疗结束后,9例(82%)患者达到CR,2例(18%)达到PR,反应率为100%。结论:对于放疗后局部复发的鼻咽癌患者,采用同步放化疗,3D-CRT同时每周使用Docetaxel是可行的,其毒性反应在可以接受的范围内,短期疗效显著。

Docetaxel的药理学研究进展

Ｄｏｃｅｔａｘｅｌ是紫杉醇类抗肿瘤药物中的一个新的有代表性的化合物。其结构和药理与紫杉醇相似，二种药物都是紫杉的提取物：ｄｏｃｅｔａｘｅｌ是欧洲紫杉的半合成品，而紫杉醇是太平洋紫杉的天然成分。然而，它们二者目前均利用紫杉针叶为原料，通过半合成方法生产...

CD40配体激活增强Docetaxel对乳腺癌细胞增殖的抑制作用

目的探讨rhCD40L联合化疗药Docetaxel对乳腺癌细胞增殖的影响。方法用MTT法测定CD40+的乳腺癌细胞株M231、M435细胞经rhCD40L+Docetaxel处理后的增殖状况;采用碘化丙啶(PI)掺入法测定细胞周期;流式细胞仪检测癌细胞膜分子CD54、CD95及CD95L表达变化。结果 rh-CD40L可抑制M231、M435增殖,合用Docetaxel时M231、M435的增殖受到进一步抑制,G1期细胞数量明显增加(P<0.05),S期细胞数量下降(P<0.05)。CD95表达上调(P<0.05),CD54、CD95L表达下调(P<0.05)。结论 rhCD40L可提高Docetaxel对乳腺癌细胞的抗肿瘤效应,其机制可能与rh-CD40L将乳腺癌细胞增殖阻滞在G1期、上调CD95、下调CD54、CD95L表达有关。

基于Doc2Vec增强特征的长文本主题聚类研究

针对新闻长文本语义表征的难点,基于Doc2Vec文档嵌入和词向量加权方式构建增强的特征表示。利用DV-sim方法和DV-tfidf方法从文档首尾部分特定词性的内容中提取增强特征,再分别与Doc2Vec文档向量组合,形成新的全局表征。DV-sim从语义角度,采用特征词与Doc2Vec向量的相似度获得词权重;DV-tfidf从词频统计角度,采用词频-逆文档频率方式获得词权重,然后利用HDBSCAN算法在THUCNews和Sogou数据集上进行主题聚类。相比直接应用Doc2Vec向量,DV-sim在两个数据集上的噪声数分别减少60.82%和60.63%,准确率提高12.14%和20.58%,F1-Score值提高15.61%和11.58%;DV-tfifd在两个数据集上的噪声数分别减少15.20%和59.55%,准确率提高10.85%和17.93%,F1-Score值提高15.60%和9.21%。实验结果表明,DV-sim和DV-tfidf都可以提高主题聚类性能,且基于语义的增强特征比基于词频的效果更好,DV-sim在优秀女性人物报道的主题聚类上也得到了有效应用。

Docetaxel治疗激素非依赖性前列腺癌的应用进展

激素非依赖性前列腺癌是泌尿糸肿瘤学中最为复杂的问题之一。Docetaxel通过诱导肿瘤细胞凋亡可达到抗肿瘤作用,因其独特的作用机制和良好的耐受性,已被广泛用于和蒽环类、吉西他滨、铂类等联合应用。该文就Docetaxel在激素非依赖性前列腺癌治疗中的进展综述如下。

Surgical outcome after docetaxel-based neoadjuvant chemotherapy in locally-advanced gastric cancer

AIM:To investigate feasibility,morbidity and surgical mortality of a docetaxel-based chemotherapy regimen randomly administered before or after gastrectomy in patients suffering from locally-advanced resectable gastric cancer.METHODS:Patients suffering from locally-advanced(T3-4 any N M0 or any T N1-3 M0)gastric carcinoma,staged with endoscopic ultrasound,bone scan,computed tomography,and laparoscopy,were assigned to receive four 21 d/cycles of TCF(docetaxel 75 mg/m 2 day 1,cisplatin 75 mg/m 2 day 1,and fluorouracil 300 mg/m 2 per day for days 1-14),either before(Arm A)or after(Arm B)gastrectomy.Operative morbidity,overall mortality,and severe adverse events were compared by intention-to-treat analysis.RESULTS:From November 1999 to November 2005,70 patients were treated.After preoperative TCF(Arm A),thirty-two(94%)resections were performed,85% of which were R0.Pathological response was complete in 4 patients(11.7%),and partial in 18(55%).No surgical mortality and 28.5%morbidity rate were observed,similar to those of immediate surgery arm(P= 0.86).Serious chemotherapy adverse events tended to be more frequent in arm B(23%vs 11%,P=0.07),with a single death per arm.CONCLUSION:Surgery following docetaxel-based chemotherapy was safe and with similar morbidity to immediate surgery in patients with locally-advanced resectable gastric carcinoma.

磷酸钙结晶与PFS混凝联用去除铜绿微囊藻和DOC

为实现藻细胞和DOC的同步高效去除,利用磷酸钙结晶预处理,强化聚合硫酸铁(PFS)混凝除藻效果,研究了磷酸钙结晶与PFS混凝联用对藻细胞和DOC的去除效果和机制,并考察了其对藻密度变化的适应性和残余磷控制的效果.结果表明,铜绿微囊藻藻密度为2.0×10^(6)cells/mL、PFS投加量为20mg/L时,Ca_(3)(PO_(4))_(2)结晶可将PFS混凝的除藻率和DOC去除率从72.5%和33.5%分别提高至91.5%和85%.Ca_(3)(PO_(4))_(2)结晶对除藻率的提升,主要通过Ca_(3)(PO_(4))_(2)均相结晶产物的共絮凝和加重剂作用来实现;对DOC去除率的提升,主要是由DOC与Ca_(3)(PO_(4))_(2)共沉淀和吸附作用实现.Ca_(3)(PO_(4))_(2)结晶与PFS联合除藻对藻细胞密度变化具有良好的适应性,且有望将残余磷浓度控制在20μg/L以下,可用于自来水厂蓝藻水华期间的应急除藻.

Prognostic factors in Chinese patients with metastatic castration-resistant prostate cancer treated with docetaxel-based chemotherapy

This study aims to evaluate the potential value of patient characteristics in predicting overall survival （OS） in patients with metastatic castration-resistant prostate cancer （mCRPC） treated with docetaxel-based thermotherapy. A total of 115 patients with mCRPC undergoing a docetaxel q3w regimen were enrolled in this study. A survival analysis was performed using the Kaplan-Meier method. Cox proportional hazards models were used to evaluate the prognostic value of all covariates for OS. OS was also analysed after stratifying patients according to the results of multivariate analysis. The median OS for the entire cohort was 17.0 months. The multivariate analysis showed that the prostate-specific antigen doubling time （PSADT）, baseline haemoglobin （Hb） concentration, alkaline phosphatase （ALP） concentration, cycles of chemotherapy and time to castration resistance were independent prognostic factors of OS. According to the presence of PSADT 〈46.3 days and baseline ALP/〉 110 IU 1-1, all patients were divided into three risk groups： low-risk group （no risk factors）, intermediate-risk group （one risk factor） and high-risk group （two risk factors）. Median OSs for patients in low-, intermediate- and high-risk groups were 28.0 months （95% Ch 23.8-32.2）, 21.0 months （95% Ch 18.9-23.1） and 11.0 months （95% Ch 7.6-14.4）, respectively （P〈O.O01）. In conclusion, PSADT, baseline Hb concentration, ALP concentration, cycles of chemotherapy and time to castration resistance were independent prognostic factors of OS in Chinese patients with mCRPC treated with docetaxel. PSADT combined with the baseline ALP concentration could be a useful risk stratification parameter for evaluating survival outcomes.

Clinical study of docetaxel combined with concurrent radiotherapy in patients with advanced nasopharyngeal carcinoma

Objective： The aim of this study was to study the short-term curative effects and adverse reactions of docetaxel （DOC） in concurrent chemoradiotherapy compared to DDP plus 5-Fu （DF） combined with concurrent radiotherapy in patients with advanced nasopharyngeal carcinoma. Methods： Thirty-three patients in the experimental group （DOC group） were given DOC 25 mg/m2 ivgtt, dl, 7 times, concurrent radiotherapy was performed from dl. Thirty-three patients in the control group （DF group） were given cisplatin 25 mg/@ivgtt dl-3 and 5-Fu 550 mg/m2iv, dl-5, 3 weeks a cycle, 2 cycles, and concurrent radiotherapy was performed from dl. Six MV X-ray and 9 MeV electronic line for external irradiation were adopted in concur- rent radiotherapy. Results： The response rates of DOC group and DF group were 90.9% and 93.9%, the rates of neutropenia were 45.45% and 67.74%, and the rates of oral mucositis were 60.61% and 90.32%. Conclusion： The difference of short- term curative effects between DOC group and DF group was not statistically significant in patients with advanced nasopha- ryngeal carcinoma. The rates of adverse reactions were lower in DOC group. DOC combined with concurrent radiotherapy could be a new choice for patients with advanced nasopharyngeal carcinoma.