重组血管生成抑制因子r—K4K5的分离纯化与功能鉴定

目的 分离纯化r-K4K5,探讨r-K4K5对牛毛血管内皮（BCE）细胞、鸡胚绒毛尿囊膜（CAM）新生血管生成及实验性人肺腺癌SPC-A1生长的抑制作用。方法 通过盐析、凝胶过滤提纯r-K4K5,BCE细胞在含r-K4K5的DMEM中培养24、48、72h后分别计数;孵化7d的鸡胚加r-K4K5后继续孵育72h,观察新生血管生成;已经接种入SPC-A1肺腺癌组织的荷瘤裸小鼠（Balb/c,nu/nu）,瘤旁注射r-K4K5继续饲养,观察肿瘤生长变化。结果 r-K4K5抑制BCE细胞增殖,48～72h作用明显;r-K4K5处理的CAM组中直径小于50um的小血管明显减少;高剂量r-K4K5治疗的荷瘤裸小鼠组,平均瘤重与对照组比较有统计学意义。结论 r-K4K5能够抑制BCE细胞增殖,抑制鸡胚CAM新生血管生成,抑制实验性人SPC-A1肺腺瘤生长。     

Efficacy and Safety of Atezolizumab Plus Bevacizumab Following Disease Progression on Atezolizumab or Sunitinib Monotherapy in Patients with Metastatic Renal Cell Carcinoma in IMmotion150: A Randomized Phase 2 Clinical Trial

BackgroundThe use of immune checkpoint inhibitors combined with vascular endothelial growth factor (VEGF)-targeted therapy as second-line treatment for metastatic clear cell renal cancer (mRCC) has not been evaluated prospectively.ObjectiveTo evaluate the efficacy and safety of atezolizumab + bevacizumab following disease progression on atezolizumab or sunitinib monotherapy in patients with mRCC.Design, setting, and participantsIMmotion150 was a multicenter, randomized, open-label, phase 2 study of patients with untreated mRCC. Patients randomized to the atezolizumab or sunitinib arm who had investigator-assessed progression as per RECIST 1.1 could be treated with second-line atezolizumab + bevacizumab.InterventionPatients received atezolizumab 1200 mg intravenously (IV) plus bevacizumab 15 mg/kg IV every 3 wk following disease progression on either atezolizumab or sunitinib monotherapy.Outcome measurements and statistical analysisThe secondary endpoints analyzed during the second-line part of IMmotion150 included objective response rate (ORR), progression-free survival (PFS), and safety. PFS was examined using Kaplan-Meier methods.Results and limitationsFifty-nine patients in the atezolizumab arm and 78 in the sunitinib arm were eligible, and 103 initiated second-line atezolizumab + bevacizumab (atezolizumab arm, n = 44; sunitinib arm, n = 59). ORR (95% confidence interval [CI]) was 27% (19–37%). The median PFS (95% CI) from the start of second line was 8.7 (5.6–13.7) mo. The median event follow-up duration was 19.4 (12.9–21.9) mo among the 25 patients without a PFS event. Eighty-six (83%) patients had treatment-related adverse events; 31 of 103 (30%) had grade 3/4 events. Limitations were the small sample size and selection for progressors.ConclusionsThe atezolizumab + bevacizumab combination had activity and was tolerable in patients with progression on atezolizumab or sunitinib. Further studies are needed to investigate sequencing strategies in mRCC.Patient summaryPatients with advanced kidney cancer whose disease had worsened during treatment with atezolizumab or sunitinib began second-line treatment with atezolizumab + bevacizumab. Tumors shrank in more than one-quarter of patients treated with this combination, and side effects were manageable.     

Safety of cyclin-dependent kinase4/6 inhibitor combined with palliative radiotherapy in patients with metastatic breast cancer

IntroductionCyclin-dependent kinase (CDK)4/6 inhibitor is a first-line therapy for metastatic ER+/HER2-breast cancer. However, there are limited data on safety of combined radiotherapy (RT) and CDK4/6 inhibition.MethodsWe conducted a retrospective study of women with metastatic breast cancer who received palliative RT within 14 days of CDK4/6 inhibitor use. The primary endpoint was toxicity per Common Terminology Criteria for Adverse Events v5. Secondary endpoints were pain response and local control based on clinical assessment and imaging.ResultsThirty patients underwent 36 RT courses with palbociclib (n = 34 courses, 94.4%) or abemaciclib (n = 2, 5.6%). RT was delivered before, concurrently or after CDK4/6 inhibitors in 7 (19.4%), 8 (22.2%), and 21 (58.3%) of cases with median 3.5 days from RT to closest CDK4/6 inhibitor administration. Median RT dose was 30Gy (range 8–40.05Gy). Treated sites included brain (n = 5, 11.6%), spine (n = 19, 44.2%), pelvis (n = 9, 20.9%), other bony sites (n = 6, 14.0%) and others (n = 4, 9.3%). No acute grade ≥3 non-hematologic toxicity occurred. No increased hematologic toxicity was attributable to RT with grade 3 hematologic toxicities rates 16.7%, 0%, and 6.7% before, during, and 2 weeks after RT completion. All but one patient (29/30) achieved symptom relief. Local control rates were 94.4%, 91.7% at 6 and 12 months.ConclusionsThe use of RT within 2 weeks of CDK4/6 inhibitors had low acceptable toxicity and high efficacy, suggesting that it is safe for palliation of metastatic breast cancer.     

ACEI对去卵巢骨质疏松大鼠激肽释放酶-激肽系统及骨丢失的影响

目的探究血管紧张素转换酶抑制剂(angiotensin-converting enzyme inhibitor,ACEI)卡托普利对去卵巢(OVX)骨质疏松大鼠骨丢失及激肽释放酶-激肽(kallikrein-kinin system,KKS)系统的影响。方法去卵巢法制备绝经骨质疏松大鼠模型,分为OVX组、ACEI组[6 mg/(kg·d)卡托普利]、阳性对照雌激素组[0.05 mg/(kg·d)己烯雌酚],另不去卵巢为Sham组。给药8周后,全自动生化分析仪检测血清钙(Ca)、Ⅰ型前胶原N-端肽(PINP)、碱性磷酸酶(ALP)、骨钙素(OCN)、抗酒石酸酸性磷酸酶(TRAP)及Ⅰ型胶原交联C端肽β序列(β-CTX)水平,微型计算机断层摄影术(micro CT)法检测骨密度及微结构,TRAP法观察骨组织破骨细胞数量,Western blot法检测骨组织中骨形态发生蛋白2(BMP2)、Runt相关转录因子2(Runx2)、组织激肽释放酶(KLK)、缓激肽受体1(B1R)及缓激肽(BK)蛋白表达。结果相较于Sham组,OVX组大鼠骨密度、骨小梁数量及厚度、骨体积分数、SMI、PINP、ALP、OCN水平、BMP2、Runx2蛋白表达均降低(P均0.05),骨小梁分离度、TRAP、β-CTX水平、破骨细胞数量、KLK、B1R及BK蛋白水平均增加(P均0.05)。相较于OVX组,ACEI组、阳性组大鼠骨密度、骨小梁数量及厚度、骨体积分数、SMI、PINP、ALP、OCN水平、BMP2、Runx2蛋白表达均增加,骨小梁分离度、TRAP、β-CTX水平、破骨细胞数量、KLK、B1R及BK蛋白水平降低(P0.05)。结论 ACEI可抑制KKS系统,降低破骨细胞活性减少骨吸收,增强成骨细胞活性增加骨形成,提高骨密度,改善骨微结构,进而改善OVX大鼠骨质疏松症状。     

Drugs affecting coagulation

The clotting cascade is a complex process and is an important survival mechanism. Major haemorrhage and thromboembolic events remain major causes of increased morbidity and mortality. Drugs affecting coagulation have primarily been utilized to treat or reduce the risk of thromboembolic events. However, the recent progress in the management of major trauma and treating coagulopathy has resulted in further research and development of drugs that improve clotting function. Knowledge of drugs used for both clinical circumstances is now required when working in anaesthesia or intensive care.     

腺苷脱氨酶抑制剂对氧反常大鼠心脏的保护作用

本文观察到腺苷脱氨酶抑制剂EHNA对离体灌流大鼠心脏氧反常性损伤有明显的作用,此外还发现在缺氧期(无氧灌流30分钟)EHNA也表现出明显的保护作用,心脏收缩幅度的降低和静息张力的升高均显著低于对照组。表明在缺氧期也可能有自由基的产生。