PARP抑制剂Olaparib对非小细胞肺癌细胞的放疗增敏作用及其机制

目的探讨聚腺苷二磷酸核糖聚合酶(PARP)抑制剂Olaparib对人非小细胞肺癌(NSCLC)细胞的放疗增敏作用及其可能的发生机制。方法以人NSCLC细胞A549细胞系为研究对象,采用CCK-8实验检测不同药物浓度梯度对细胞的增殖抑制作用。选择对细胞10%抑制浓度(IC10)作为后续实验的药物浓度,实验分为对照组、Olaparib组、单纯放疗组(RT组)、Olaparib联合放疗组(Olaparib+RT组)。通过克隆形成实验和EDU细胞增殖实验检测Olaparib联合放疗后的增敏效果,流式细胞术检测各组细胞周期分布,Western blot实验检测各组DNA损伤标志蛋白γ-H2AX的表达。结果Olaparib对A549细胞具有抑制作用且呈剂量依赖性;在处理A549细胞24 h后IC10为2.593μmol·L^(-1);Olaparib放疗增敏比为1.966。Olaparib+RT组A549细胞的增殖能力下降(P<0.01);Olaparib+RT组的G2/M期细胞占比高于对照组(46.0%vs 10.8%,P<0.05);且Olaparib+RT组细胞中γ-H2AX明显高于RT组(P<0.01)。结论Olaparib对人NSCLC细胞A549细胞系有着放疗增敏效果,其机制可能与影响细胞周期、增加放疗后细胞DNA双链断裂形成相关。

Olaparib对HL-60细胞NKG2D配体表达的调节作用及相关机制研究

目的:研究Olaparib对人急性髓系白血病细胞株HL-60细胞表面NKG2D配体表达的调节作用,并初步探索其内在调控机制。方法:对数生长期的HL-60细胞经不同浓度Olaparib(1.25、2.5、5、10μmol/L)作用24、48 h后,采用流式细胞术检测细胞表面NKG2D配体表达情况;Western blot检测HL-60细胞内ERK蛋白表达变化情况;CFSE/PI法检测NK细胞对HL-60细胞的杀伤作用。结果:10μmol/L Olaparib作用24和48 h均可上调HL-60细胞表面NKG2D配体的表达,5μmol/L Olaparib作用48 h可诱导ULBP-2、ULBP-3表达上调;Western blot检测结果显示,Olaparib处理后的HL-60细胞内ERK磷酸化水平增强。Olaparib可增强NK细胞对HL-60细胞的杀伤作用,但ERK抑制剂可下调NK细胞对HL-60细胞的杀伤作用。结论:Olaparib可上调HL-60细胞表面NKG2D配体表达,增强NK细胞对其的杀伤作用,其机制可能与Olaparib促进ERK磷酸化表达有关。

PARP抑制剂olaparib对急性髓系白血病细胞HL-60抑制作用研究

目的研究PARP抑制剂olaparib对人急性髓系白血病细胞株HL-60细胞的抑制作用。方法对数生长期HL-60细胞经不同浓度(0、1.25、2.5、5、10μmol/L)olaparib作用不同时间后,CCK-8法检测olaparib对HL-60细胞的增殖抑制作用;Annexin-V/PI双标法检测HL-60细胞凋亡水平,Western blot检测HL-60细胞内相关信号蛋白(PARP-1、Caspase-3)表达变化。结果与对照组相比,经不同浓度(1.25、2.5、5、10μmol/L)olaparib作用48 h后的HL-60细胞出现增殖抑制,并且随着作用时间的延长,抑制率逐渐增加;同时发现olaparib诱导HL-60细胞发生凋亡,并显示出剂量依赖效应;Western blot结果显示,olaparib处理后的HL-60细胞内PARP活性受到抑制,Caspase-3活化。结论PARP抑制剂olaparib对HL-60细胞不仅具有增殖抑制作用,同时可通过激活Caspase-3,抑制PARP活性,诱导HL-60细胞凋亡。

The New England Journal of Medicine:Olaparib,前列腺癌精准治疗里程碑

一项重要的新的临床试验证实,最初研发用于治疗罹患遗传性癌症妇女的一种开拓性药物,也可以让晚期前列腺癌患者受益。这一试验是前列腺癌治疗的一个里程碑,它第一次证实了“精准医疗”——采取与患者肿瘤特殊遗传特征相匹配的疗法对前列腺癌有好处。试验结果最近由英国癌症研究院和皇家Marsden NHS信托基金会的研究人员领导的一个国际团队发表在《新英格兰医学杂志》（MATEO J,CARREIRA S, SANDHU S, et al. the New Eng J Med, 2015,373： 1697-1708）上。

Response of BRCA1-mutated gallbladder cancer to olaparib: A case report

gallbladder cancer(gbc), although considered as a relatively rare malignancy, is the most common neoplasm of the biliary tract system. the late diagnosis and abysmal prognosis present challenges to treatment. the overall 5-year survival rate for metastatic gbc patients is extremely low. BRC A1 and BRCA2 are the breast cancer susceptibility genes and their mutation carriers are at a high risk for cancer development, both in men and women. Olaparib, an oral poly ADP-ribose polymerase inhibitor, has been approved by the Food and Drug Administration and the European commission for the treatment of ovarian cancer with any BRCA1/2 mutations. the first case of BRCA1-mutated gbc patient who responded to olaparib treatment is reported here.

Retrospective efficacy analysis of olaparib combined with bevacizumab in the treatment of advanced colorectal cancer

BACKGROUND Colorectal cancer(CRC)is a highly prevalent malignancy of the digestive tract worldwide,characterized by a significant morbidity and mortality rate and subtle initial symptoms.Diarrhea,local abdominal pain,and hematochezia occur with the development of cancer,while systemic symptoms such as anemia and weight loss occur in patients with advanced CRC.Without timely interventions,the disease can have fatal consequences within a short span.The current therapeutic options for colon cancer include olaparib and bevacizumab,which are widely utilized.This study intends to evaluate the clinical efficacy of olaparib combined with bevacizumab in the treatment of advanced CRC,hoping to provide insights into advanced CRC treatment.AIM To investigate the retrospective efficacy of olaparib combined with bevacizumab in the treatment of advanced CRC.METHODS A retrospective analysis was conducted on a cohort of 82 patients with advanced colon cancer who were admitted to the First Affiliated Hospital of the University of South China between January 2018 and October 2019.Among them,43 patients subjected to the classical FOLFOX chemotherapy regimen were selected as the control group,and 39 patients undergoing treatment with olaparib combined with bevacizumab were selected as the observation group.Subsequent to different treatment regimens,the short-term efficacy,time to progression(TTP),and incidence rate of adverse reactions between the two groups were compared.Changes in serum-related indicators[vascular endothelial growth factor(VEGF),matrix metalloprotein-9(MMP-9),cyclooxygenase-2(COX-2)]and tumor markers[human epididymis protein 4(HE4),carbohydrate antigen 125(CA125),carbohydrate antigen 199(CA199)]levels before and after treatment were compared between the two groups at the same time.RESULTS The objective response rate was discovered to be 82.05%,and the disease control rate was 97.44%in the observation group,which were significantly higher than the respective rates of 58.14%and 83.72%in the control group(P<0.05).The median TTP was 24 mo(95%CI:19.987-28.005)in the control group and 37 mo(95%CI:30.854-43.870)in the observation group.The TTP in the observation group was significantly better than that in the control group,and the difference held statistical significance(log-rank test value=5.009,P=0.025).Before treatment,no substantial difference was detected in serum VEGF,MMP-9,and COX-2 levels and tumor markers HE4,CA125,and CA199 levels between the two groups(P>0.05).Following treatment with different regimens,the above indicators in the two groups were remarkably promoted(P<0.05),VEGF,MMP-9,and COX-2 in the observation group were lower than those in the control group(P<0.05),and HE4,CA125,and CA199 levels were also lower than those in the control group(P<0.05).Visà-vis the control group,the total incidence of gastrointestinal reactions,thrombosis,bone marrow suppression,liver and kidney function injury,and other adverse reactions in the observation group was notably lowered,with the difference considered statistically significant(P<0.05).CONCLUSION Olaparib combined with bevacizumab in the treatment of advanced CRC demonstrates a strong clinical effect of delaying disease progression and reducing the serum levels of VEGF,MMP-9,COX-2 and tumor markers HE4,CA125 and CA199.Moreover,given its fewer adverse reactions,it can be regarded as a safe and reliable treatment option.

Impact of Olaparib for Maintenance Monotherapy on Survival in Breast and Ovarian Cancer: A Systematic Review and Pooled Analysis of Published Trials

Purpose: To assess the efficacy and safety of Olaparib, a PARP inhibitor on progression-free survival (PFS), objective response rate (ORR) and overall survival (OS) in patients with breast and ovarian cancer. Methods: Research data from clinical trials through PubMed, Science Citation Index, Elsevier Science Direct and Cochrane Library of all published studies exploring the PFS, ORR or OS of Olaparib for maintenance monotherapy on survival in breast and ovarian cancer were analysed. Pooled estimates of the ORR, weighted medians of PFS and OS from all Olaparib were calculated. Assessment of quality and level of evidence was assigned by Cochrane guidelines and guidelines of Oxford Centre for Evidence-Based Medicine. Results: Data of 893 patients (731 olaparib;162 control) from 6 trials, 2 randomised controlled trials and 4 non-randomised trials, were included. The overall median weighted PFS and OS in patients treated with Olaparib were 5.9 and 19.1 months, respectively. The pooled ORR was 25%. Olaparib showed a greater effect on PFS in patients with both wild-type BRCA and BRCA mutant gene. The most common toxicity were nausea and vomiting. Conclusions: Olaparib as maintenance monotherapy for breast and ovarian cancer is associated with promising outcomes including increased response rate and improved PFS. Its potential in clinical application is needed for further investigation in phase III trials.

Pancreatic mucinous cystadenocarcinoma in a patient harbouring BRCA1 germline mutation effectively treated with olaparib: A case report

BACKGROUND Pancreatic mucinous cystadenocarcinoma(MCAC)is a rare malignancy with a poor prognosis when it presents metastases at diagnosis.Due to its very low incidence,there are no clear recommendations for the treatment of advanced disease.Olaparib(an oral PARP inhibitor)has been approved for the maintenance treatment of patients with metastatic pancreatic adenocarcinoma harbouring germline BRCA1/2 mutations.Herein,we report the first case of a germline BRCA1 mutated unresectable MCAC which was effectively treated with olaparib.CASE SUMMARY A 41-year-old woman,without personal or family history of cancer,was diagnosed with ovarian and peritoneal metastases of MCAC.She underwent 12 cycles of gemcitabine plus oxaliplatin(GEMOX)obtaining a partial response and allowing radical surgery.One year later,local recurrence was documented,and other 12 cycles of GEMOX were administered obtaining a complete response.Seven years later,another local recurrence,not amenable to surgical resection,was diagnosed.She started FOLFIRINOX(oxaliplatin,irinotecan,leucovorin and fluorouracil),obtaining a partial response after 8 cycles.Given the excellent response to platinum-based chemotherapy,BRCA testing was performed,and a BRCA1 germline mutation was detected.She was switched to maintenance olaparib due to chemotherapy-related toxicities and achieved an almost complete metabolic response,with a reduction in the diameter of the lesion,after three months of therapy.CONCLUSION The current case suggests the beneficial effect of olaparib in BRCA mutated MCAC.However,further studies are required.

Circulating tumor DNA genomic profiling reveals the complicated olaparib-resistance mechanism in prostate cancer salvage therapy: A case report

BACKGROUND The poly(ADP-ribose)polymerase(PARP)inhibitor olaparib has displayed superior clinical effect in metastatic castration-resistant prostate cancer(mCRPC)patients with the homologous recombination repair(HRR)genes mutations.However,when a patient’s tumor tissue volume is insufficient for genomic profiling of HRR gene mutations,circulating tumor DNA(ctDNA)may be useful in helping to determine and monitor the efficacy of olaparib,as well as in abiraterone-combination treatment,and for understanding any resistance mechanism related to such mutations.CASE SUMMARY A 61-year-old man who was diagnosed with metastatic prostate adenocarcinoma was initially hormone sensitivity,showing high Gleason score(5+5=10)and absolute positive rate(14/14 biopsied specimens).Following failure of several standard therapies,the patient progressed to mCRPC.Surprisingly,the patient showed good response to olaparib-abiraterone-prednisone combination treatment(an androgen-deprivation therapy,provided as the‘final choice’in China).Serum total prostate-specific antigen(TPSA)level reduced and symptoms remitted for 4 months.However,thereafter,serum TPSA levels began slowly increasing,indicating development of olaparib resistance.Subsequent comprehensive genomic profiling of ctDNA, screening 508 cancer-related genes by next-generation sequencing,identified 10 somatic variants as well as 3 copy number alterations. Two identified reversemissense mutations in partner and localizer of BRCA2 (PALB2) may have recovered the readingframe, restoring function of the primary germline PALB2 mutation and causing resistance to thePARP inhibitor olaparib.CONCLUSIONReverse mutations in PALB2, discovered via genomic profiling of ctDNA, may represent apotential resistance mechanism against olaparib in mCRPC.

美国FDA批准Lynparza(olaparib)用于治疗晚期卵巢癌

美国FDA于2014年12月19日批准Lynparza（olaparib）用于治疗因BRCA基因（gB RCAm）突变引起的晚期卵巢癌。FDA同时批准了一种对BRCA基因突变进行检测的仪器,名为BRACAnalysis CDx。 BRCA基因可以修复受损的DNA,抑制肿瘤细胞的生长。发生BRCA基因突变的女性更容易患卵巢癌。据估计，约10％～15％的卵巢癌患者与这种遗传性的BRCA基因突变有关。经BRACAnalysis CDx检测确认有BRCA基因突变的卵巢癌患者可接受Lynparza治疗。

阿斯利康PARP抑制剂Lynparza(olaparib)获得欧盟委员会批准

近日,阿斯利康宣布其PARP抑制剂Lynparza(olaparib)获得欧盟委员会批准作为一线维持疗法,用于BRCA突变的晚期卵巢癌患者。Lynparza是全球上市的首个PARP抑制剂,2014年12月首次获得美国FDA批准用于携带有害或疑似有害种系BRCA突变(gBRCAm)的晚期卵巢癌患者。2018年12月获得美国FDA的批准作为一线维持治疗BRCAm晚期卵巢癌。

Bibliometric analysis of olaparib and pancreatic cancer from 2009 to 2022:A global perspective

BACKGROUND Genetic screening for breast cancer gene 1(BRCA)1/2 mutations can inform breast/ovarian/pancreatic cancer patients of suitable therapeutic interventions.Four to seven percent of pancreatic cancer patients have germline BRCA mutations.BRCA genes aid in DNA repair,especially homologous recombination,which impacts genomic stability and cancer cell growth.BRCA1 regulates the cell cycle,ubiquitination,and chromatin remodeling,whereas BRCA2 stimulates the immune response.They predict the efficacy of platinum chemotherapy or polymerase(PARP)inhibitors such as olaparib.AIM To determine the trends and future directions in the use of olaparib for pancreatic cancer treatment.METHODS To evaluate the trends in how olaparib works in pancreatic cancer,we performed a bibliometric analysis.One hundred and ninety-six related publications were accessed from the Web of Science Core Collection and were published between 2009 and 2022.The analytic parameters included publications,related citations,productive countries and institutes,influential authors,and keyword development.RESULTS This study visualizes and discusses the current research,including the present global trends and future directions in olaparib and pancreatic cancer.Overall,this study sheds light on optimizing the use of olaparib in pancreatic cancer treatment,Feng X et al.The use of olaparib in pancreatic cancer WJGO https://www.wjgnet.com 4490 November 15,2024 Volume 16 Issue 11 offering valuable guidance for researchers in this field.CONCLUSION Our findings identified trends in olaparib and pancreatic cancer,with China and the USA leading and with global cooperation tightening.O'Reilly EM's team and Memorial Sloan-Kettering had the highest output.The Journal of Clinical Oncology was the most cited journal.More PARP inhibitors are emerging,and combination therapy is suggested for future therapeutic trends.

PARP抑制剂olaparib

olaparib是一种聚腺苷二磷酸核糖聚合酶(PARP)抑制剂,能选择性地作用于BRCA突变阳性的肿瘤细胞,利用"协同致死性"机制使肿瘤细胞因双链DNA损伤无法修复而死亡。2014年12月,欧盟和美国先后批准其上市,用于治疗BRCA基因突变阳性的晚期卵巢癌患者,疗效显著,不良反应少,患者短期耐受性良好,具有广泛的应用前景。现对其药理作用、药动学、药物相互作用、临床试验以及不良反应等方面进行综述。

Synthesis of Olaparib Derivatives and Their Antitumor Activities

A series of Olaparib derivatives was synthesized, and their structures were confirmed by 1H NMR, MS and elemental analysis. Their antitumor activities on breast cancer susceptbility gene 1/2（BRCAl/2）-deficient cancer cell lines including HCC1937, Capan-1 and MDA-MB-436 were evaluated. The antitumor activity of compound Olaparib-1 was better than the positive control Olaparib in BRCAl-deficient cell line HCC1937.

Enzalutamide and olaparib synergistically suppress castration-resistant prostate cancer progression by promoting apoptosis through inhibiting nonhomologous end joining pathway

Recent studies revealed the relationship among homologous recombination repair(HRR),androgen receptor(AR),and poly(adenosine diphosphate-ribose)polymerase(PARP);however,the synergy between anti-androgen enzalutamide(ENZ)and PARP inhibitor olaparib(OLA)remains unclear.Here,we showed that the synergistic effect of ENZ and OLA significantly reduced proliferation and induced apoptosis in AR-positive prostate cancer cell lines.Next-generation sequencing followed by Gene Ontology and Kyoto Encyclopedia of Genes and Genomes enrichment analyses revealed the significant effects of ENZ plus OLA on nonhomologous end joining(NHEJ)and apoptosis pathways.ENZ combined with OLA synergistically inhibited the NHEJ pathway by repressing DNA-dependent protein kinase catalytic subunit(DNA-PKcs)and X-ray repair cross complementing 4(XRCC4).Moreover,our data showed that ENZ could enhance the response of prostate cancer cells to the combination therapy by reversing the anti-apoptotic effect of OLA through the downregulation of anti-apoptotic gene insulin-like growth factor 1 receptor(IGF1R)and the upregulation of pro-apoptotic gene death-associated protein kinase 1(DAPK1).Collectively,our results suggested that ENZ combined with OLA can promote prostate cancer cell apoptosis by multiple pathways other than inducing HRR defects,providing evidence for the combined use of ENZ and OLA in prostate cancer regardless of HRR gene mutation status.

奥拉帕尼诱导乳腺癌MCF-7细胞衰老作用及其机制

目的 研究奥拉帕尼(olaparib)诱导乳腺癌MCF-7细胞衰老作用的表现及其相关分子水平作用机制。方法 利用实时细胞分析(real-time cell analysis, RTCA)技术实时动态检测抗增殖和抗迁移活性;应用衰老相关β-半乳糖苷酶(senescence-associated β-galactosidase, SA-β-gal)染色法观察诱导细胞衰老活性;通过qPCR分析奥拉帕尼对衰老相关基因p16、p21、C/EBP同源蛋白(C/EBP homologous protein, CHOP)、白细胞介素(interleukin, IL)-6、IL-8、纤溶酶原激活物抑制剂-1(plasminogen activator inhibitor 1,PAI-1)、磷酸酶和张力蛋白同源物(phosphatase and tensin homolog deleted on chromosome 10,PTEN)、p27、视网膜母细胞瘤基因(retinoblastoma gene, RB1)、Ki67和E2F1表达的影响;根据Western Blot分析奥拉帕尼对衰老相关蛋白p21、γH2AX、胰岛素样生长因子结合蛋白3(insulin-like growth factor binding protein 3,IGFBP3)、cyclin D1、pRB和Ki67表达的影响。结果 奥拉帕尼能够抑制乳腺癌MCF-7细胞增殖、迁移并诱导MCF-7细胞的衰老;奥拉帕尼作用96 h的MCF-7细胞中p16、p21、p27、CHOP、IL-6、IL-8、PAI-1、PTEN和RB1的基因表达水平显著上调(P<0.01),Ki67和E2F1的基因表达水平显著下调(P<0.01);MCF-7细胞中p21、γH2AX和IGFBP3蛋白的表达水平显著升高(P<0.01,P<0.01,P<0.05),cyclin D1、pRB和Ki67蛋白的表达水平显著降低(P<0.05,P<0.01,P<0.05)。结论 奥拉帕尼能够通过抗增殖、迁移和诱导细胞衰老产生抗乳腺癌MCF-7细胞作用。

奥拉帕利对铂敏感复发BRCA突变卵巢癌患者PD-1/PD-L1信号通路的影响

目的探讨奥拉帕利与含铂方案对铂敏感复发乳腺癌易感基因(BRCA)突变卵巢癌(OC)患者肿瘤血管生成相关因子及程序性死亡受体-1(PD-1)/程序性死亡-配体1(PD-L1)信号通路的影响。方法回顾性选取2018年5月至2020年5月该院95例铂敏感复发BRCA突变OC患者,依据治疗方案不同分为两组,对照组47例接受紫杉类+铂类治疗,观察组48例接受奥拉帕利片。对比两组疗效、安全性、肿瘤血管生成相关因子[血管生成素-2(Ang-2)、血管内皮生长因子(VEGF)、基质细胞衍生因子-1α(SDF-1α)]、外周血CD4^(+)T细胞PD-1、PD-L1水平。结果观察组DCR比对照组高,差异有统计学意义(P<0.05)。观察组恶心、疲劳与乏力、呕吐、贫血、腹泻、白细胞减少、中性粒细胞减少及食欲减退发生率与对照组比较,差异无统计学意义(P>0.05)。观察组治疗3、6个周期血清VEGF、Ang-2及SDF-1α水平低于对照组,差异有统计学意义(P<0.05)。观察组治疗3、6个周期外周血CD4^(+)T细胞PD-1、PD-L1水平低于对照组,差异有统计学意义(P<0.05)。结论奥拉帕利应用于铂敏感复发BRCA突变OC患者中,可调控PD-1/PD-L1信号通路,降低肿瘤血管生成相关因子水平,提升治疗效果。

大黄蛰虫丸加减联合奥拉帕利治疗乳腺癌基因突变型卵巢癌

目的研究大黄蛰虫丸加减联合奥拉帕利治疗乳腺癌基因(breast cancergene,BRCA)突变型卵巢癌的疗效及对癌胚抗原(car-cinoembryonic antigen,CEA)、糖类抗原125(carbohydrate antigen 125,CA125)、糖类抗原199(carbohydrate antigen 199,CA199)水平的影响。方法纳入2021年2月至2023年2月在河南中医药大学第三附属医院进行手术治疗的98例卵巢癌患者的临床资料,根据治疗方式将患者分为对照组(n=49)和观察组(n=49),对照组采用奥拉帕利进行干预,观察组采用大黄蛰虫丸加减联合奥拉帕利进行干预,观察两组治疗前后临床疗效、肿瘤标志物CEA、CA125、CA199水平和药物不良反应。结果治疗后观察组CEA、CA125、CA199水平低于对照组(P<0.05);观察组治疗期间的恶心、肝肾功能异常、疼痛发生率均低于对照组(P<0.05);治疗前两组中医症候(小腹胀痛、纳差、面色晦暗)评分差异无统计学意义(P>0.05);治疗后,两组小腹胀痛、纳差、面色晦暗评分均降低,且观察组评分低于对照组(P<0.05);观察组西医治疗有效率(83.67%)高于对照组(55.10%)(P<0.05);对照组中医治疗有效率(53.06%)低于观察组(83.67%)(P<0.05)。结论大黄蛰虫丸加减联合奥拉帕利治疗BRCA突变型乳腺癌能够起到提高临床疗效、减少药物不良反应的作用。

Low testing rates and high BRCA prevalence: Poly (ADP-ribose) polymerase inhibitor use in Middle East BRCA/homologous recombination deficiency-positive cancer patients

BACKGROUND Poly(ADP-ribose)polymerase inhibitors(PARPis)are approved as first-line therapies for breast cancer gene(BRCA)-positive,human epidermal growth factor receptor 2-negative locally advanced or metastatic breast cancer.They are also effective for new and recurrent ovarian cancers that are BRCA-or homologous recombination deficiency(HRD)-positive.However,data on these mutations and PARPi use in the Middle East are limited.AIM To assess BRCA/HRD prevalence and PARPi use in patients in the Middle East with breast/ovarian cancer.METHODS This was a single-center retrospective study of 57 of 472 breast cancer patients tested for BRCA mutations,and 25 of 65 ovarian cancer patients tested for HRD.These adult patients participated in at least four visits to the oncology service at our center between August 2021 and May 2023.Data were summarized using descriptive statistics and compared using counts and percentages.Response to treatment was assessed using Response Evaluation Criteria in Solid Tumors criteria.RESULTS Among the 472 breast cancer patients,12.1%underwent BRCA testing,and 38.5%of 65 ovarian cancer patients received HRD testing.Pathogenic mutations were found in 25.6%of the tested patients:26.3%breast cancers had germline BRCA(gBRCA)mutations and 24.0%ovarian cancers showed HRD.Notably,40.0%of gBRCA-positive breast cancers and 66.0%of HRD-positive ovarian cancers were Middle Eastern and Asian patients,respectively.PARPi treatment was used in 5(33.3%)gBRCA-positive breast cancer patients as first-line therapy(n=1;7-months progression-free),for maintenance(n=2;>15-months progression-free),or at later stages due to compliance issues(n=2).Four patients(66.6%)with HRD-positive ovarian cancer received PARPi and all remained progression-free.CONCLUSION Lower testing rates but higher BRCA mutations in breast cancer were found.Ethnicity reflected United Arab Emirates demographics,with breast cancer in Middle Eastern and ovarian cancer in Asian patients.

奥拉帕利对内毒素致急性肺损伤小鼠的保护作用

目的探讨奥拉帕利对内毒素致急性肺损伤小鼠的保护作用。方法24只SPF级雄性C57BL/6小鼠,8~10周龄,体质量20~30 g,按随机数字表法分为4组(n=6):control组、脂多糖(lipopolysaccharide,LPS)组、5 mg/kg奥拉帕利组和10 mg/kg奥拉帕利组。LPS组、5 mg/kg奥拉帕利组和10 mg/kg奥拉帕利组采用1 mg/mL LPS雾化构建ALI模型,每天30 min,连续3 d。5 mg/kg奥拉帕利组和10 mg/kg奥拉帕利组在第3天雾化后,即刻分别腹腔注射5,10 mg/kg奥拉帕利;control组腹腔注射等量生理盐水。给药后观察小鼠行为改变等一般情况,并于给药后24 h后处死小鼠,检测肺湿/干重比;BCA法分别测定血清和肺泡灌洗液总蛋白的含量,计算肺通透性指数(lung pemeability index,LPI);ELISA法测肺组织和血清IL-6、TNF-α、IL-1β的浓度;酶比色法测肺组织脂质过氧化丙二醛(malondialdehyde,MDA)和总抗氧化能力(total antioxidant capacity,T-AOC)的含量、超氧化物歧化酶(superoxide dismutase,SOD)和髓过氧化物酶(myeloperoxidase,MPO)的活性;HE染色测定肺组织损伤程度评分;免疫组化评估肺组织Caspase-1的表达水平。结果腹腔注射奥拉帕利后可见小鼠均存活,精神较前无明显烦躁及萎靡,无恶心、呕吐、腹泻、食欲减退等症状。与control组比较,LPS组、5 mg/kg奥拉帕利组和10 mg/kg奥拉帕利组肺湿/干比、LPI显著升高(P<0.05),肺组织和血清IL-6、TNF-α、IL-1β浓度显著升高(P<0.05),肺组织MDA的含量和MPO的活性显著升高(P<0.05),肺组织SOD的活性和T-AOC的含量显著下降(P<0.05),肺组织Caspase-1的表达水平显著升高(P<0.05),肺组织病理学损伤评分显著升高(P<0.05)。与LPS组比较,5 mg/kg奥拉帕利组和10 mg/kg奥拉帕利组肺湿/干比、LPI显著降低(P<0.05),肺组织和血清IL-6、TNF-α、IL-1β浓度显著降低(P<0.05),肺组织MDA的含量和MPO的活性显著降低(P<0.05),SOD的活性和T-AOC的含量显著升高(P<0.05),Caspase-1的表达水平显著降低(P<0.05),肺组织病理学损伤评分显著降低(P<0.05)。与5 mg/kg奥拉帕利组比较,10 mg/kg奥拉帕利组肺湿/干比、LPI显著降低(P<0.05),肺组织和血清IL-6、TNF-α、IL-1β浓度显著降低(P<0.05),MDA的含量和MPO的活性显著降低(P<0.05),SOD的活性和T-AOC的含量显著升高(P<0.05),Caspase-1的表达水平显著降低(P<0.05),肺组织病理学损伤评分显著降低(P<0.05)。结论腹腔注射奥拉帕利能够减轻内毒素致ALI小鼠肺部及全身炎症反应、肺水肿、肺组织损伤,降低肺组织氧化应激水平,通过抑制Caspase-1/IL-1β信号通路减轻细胞焦亡,且剂量为10 mg/kg时未见明显不良反应,疗效更佳。