Diagnostic approach to well-differentiated hepatocellular carcinoma

Well-differentiated hepatocellular mass-lesions in non-cirrhotic livers have a differential diagnosis of focal nodular hyperplasia, regenerative hepatic pseudotumors, hepatic adenoma, hepatocellular carcinoma, and fibrolamellar carcinoma. Despite significant advances in characterizing these pseudotumors and tumors, they remain a diagnostic challenge, especially on needle biopsy. This review focuses on a systematic diagnostic approach, one that allows confident diagnosis of these lesions.     

非小细胞肺癌组织Ki-67 与PD-L1 表达的相关性及其对患者预后的影响

[摘要] 目的：探讨NSCLC患者癌组织中Ki-67 与PD-L1 表达的相关性及两者对患者预后的影响。方法：选取符合纳入标准的2012 年1 月至2018 年8 月在海军军医大学附属长海医院，手术确诊为NSCLC并进行免疫组化PD-L1 和Ki-67 检测的患者401 例，收集其临床病理资料，定期生存随访，应用统计学方法分析Ki-67 与PD-L1 表达的相关性及两者对患者术后DFS和化疗后PFS的影响。结果：NSCLC组织中PD-L1 和Ki-67 表达阳性率分别为37.9%（152/401）和96.3%（386/401），单因素分析显示Ki-67 为PDL1表达相关的影响因素（OR=0.33，95%CI=0.28～0.39，P<0.0001），曲线拟合分析显示Ki-67 与PD-L1 表达显著正相关，阈值效应分析、分段多因素Logistic 和ROC曲线分析表明14%是Ki-67 较适宜与PD-L1 联用的阈值。Kaplan-Meier 分析显示，术后DFS，Ki-67 高表达组显著短于Ki-67 低表达组[(21.88±11.25) vs (41.22±16.25)个月，P<0.0001]，PD-L1 阳性组显著短于PD-L1 阴性组[(24.75±14.59) vs (38.27±16.75)个月，P<0.0001]，Ki-67 高表达/PD-L1 阳性组与其余3 组相比术后DFS 最短[(20.57±11.33) vs(24.11±10.79) vs (36.00±16.79) vs (42.91±15.77)个月，P<0.0001]；化疗PFS，Ki-67 高表达组显著长于Ki-67 低表达组[(7.70±3.01) vs(5.80±2.99)个月，P=0.016]，PD-L1 阳性组与阴性组相比差异无统计学意义[(7.04±3.21) vs (6.33±3.06)个月，P=0.22]，Ki-67 与PDL1联合测评，Ki-67 高表达两组的PFS显著长于Ki-67 低表达两组[(7.74±3.25) vs (7.43±2.38) vs(4.91±1.97) vs (6.02±3.19)个月，P=0.041]。结论：NSCLC组织中Ki-67 与PD-L1 表达呈正相关，Ki-67 14%是适宜与PD-L1 联用的阈值，Ki-67 和PD-L1 均为患者预后不良的预测因子，两者联合对预后不良的预测有“叠加效应”，同时Ki-67 高表达患者对化疗的敏感性较好。     

Mechanistic perspective of protective effects of nilotinib against cisplatin-induced testicular injury in rats: Role of JNK/caspase-3 signaling inhibition

Cisplatin is an effective anticancer used widely in treatment of solid and germ cell tumors, however, the immense toxicity on healthy tissues discourages cisplatin use in prolonged treatment protocols. Testicular toxicity is amongst its undesired adverse effects. Nilotinib is a second generation multityrosine kinase inhibitor which is used as an anticancer agent with anti-inflammatory and antioxidant activities. In the present study, a single dose of cisplatin (7 mg/kg, I.P) to rats induced a significant testicular injury. Daily administration of nilotinib (20 mg/kg, orally) 24 h post cisplatin injection for 10 days ameliorated testicular damage. Nilotinib significantly increased serum testosterone and sperm concentration outside frame of oligospermia with simultaneous full recovery of sperm viability. Nevertheless, biomarkers of apoptosis such as JNKs and Caspase -3, were significantly reduced. Moreover, improved antioxidant status of the testes was inferred by significant elevation of GSR, SOD and TAC alongside with reduction in lipid peroxidation biomarkers; MDA and 4-HNE. Flow Cytometry analysis of the cell cycle confirmed a significant increase in the percentage of testicular cells present in G2/M phase and a significant decrease in the percentage of apoptotic testicular cells after nilotinib administration. Histopathologically, nilotinib preserved testicular architecture showing significant numbers of sperm and spermatids within lumens of seminiferous tubule. Furthermore, nilotinib enhanced testicular expression of Ki67 significantly, providing evidence of testicular regeneration. In conclusion, nilotinib refinement of cisplatin induced testicular toxicity is attributed to enhancing antioxidant capabilities, decreasing apoptotic signals and restoring regenerative capacity of testes suggesting nilotinib to be used in conjunction with cisplatin in treatment protocols to avoid cisplatin induced long term testicular toxicity.     

中性粒细胞与淋巴细胞比值对三阴性乳腺癌临床预后及与Ki - 67表达的影响

目的 探讨中性粒细胞与淋巴细胞比值（neutrophil to lymphocyte ratio，NLR）对三阴性乳腺癌的临床预后影响及与Ki - 67表达的关系。方法 回顾性分析2006年1月 - 2012年12月于我院乳腺外科住院治疗的134例三阴性乳腺癌患者。NLR最佳临床分界值采用ROC曲线确定，并依此分NLR＜2.64组和NLR≥2.64组。临床独立预后因素采用单因素和多因素Cox回归模型分析。术后生存时间和生存曲线比较采用Kaplan - Meier和log - rank方法。Ki - 67的表达采用免疫组织化学方法检测。结果 NLR是三阴性乳腺癌的独立预后因素，最佳临界值为2.64。NLR＜2.64组术后中位DFS为39.10月，中位OS为52.30月；NLR≥2.64组术后中位DFS为27.35月，中位OS为37.35月。2组术后DFS和OS比较，差异具有统计学意义（P＜0.05）。NLR低组伴Ki - 67表达阴性的三阴性患者术后中位DFS和OS生存时间显著高于其他情况。结论 NLR是三阴性乳腺癌的关键影响预后因素，具有重复性强、非侵袭性、方便实用等特性，可用于预测三阴性乳腺癌临床预后。     

Development of a Nomogram to Predict the Recurrence Score of 21-Gene Prediction Assay in Hormone Receptor–Positive Early Breast Cancer

IntroductionA 21-gene prediction assay (Oncotype DX) is helpful to estimate benefit from adjuvant chemotherapy in patients with hormone receptor–positive, lymph node–negative early breast cancer. This study was conducted to develop a model to estimate high recurrence score (RS) using easily available clinicopathologic parameters in limited-resource countries.Patients and MethodsHormone receptor–positive, lymph node–negative early breast cancer patients who underwent Oncotype DX were enrolled onto the training set (n = 192). The risk category range of the RS was the same as in the TAILORx study. The multivariable logistic regression model was used to identify significant variables associated with high RS. The independent validation set (n = 264) was established from patients of a different time period.ResultsThe median age in the training set was 47 years, and 78.0% were premenopausal. The number of patients with low RS (< 11), intermediate RS (11-25), and high RS (> 25) were 42 (22.0%), 122 (63.9%), and 27 (14.1%), respectively. High nuclear grade, no progesterone receptor expression, and high Ki-67 were associated with high RS, and these variables were used to construct the nomogram. It had significant discriminatory power in internal validation (area under the curve = 0.856) and in the validation set (area under the curve = 0.828). The calibration plot showed optimal agreement between predicted and actual probabilities in both sets.ConclusionA nomogram was successfully developed with 3 simple parameters. The probability of high RS can be easily and conveniently estimated using our nomogram. It might be useful to determine whether or not Oncotype DX is conducted in the TAILORx era. Future large-scale prospective studies are warranted.     

乳腺癌缺氧诱导因子-1α、Ki-67表达与超声声像特征的关系

目的探讨乳腺癌患者乳腺癌组织中的缺氧诱导因子-1α(HIF-1α)、Ki-67蛋白的表达与超声声像特征的关系。方法对110例乳腺癌患者进行超声检查,观察患者的毛刺征、肿块形态、钙化灶形态和血流显像分级等。取110例乳腺癌患者的乳腺癌组织,免疫组化法检测HIF-1α、Ki-67蛋白的阳性表达率。分析不同超声声像特征乳腺癌患者乳腺癌组织中HIF-1α、Ki-67蛋白的表达情况。结果110例乳腺癌患者中,43例既存在Ki-67蛋白阳性表达又存在HIF-1α蛋白阳性表达,35例仅存在Ki-67蛋白阳性表达,13例仅存在HIF-1α蛋白阳性表达,Ki-67、HIF-1α蛋白阴性表达患者共19例。乳腺癌患者乳腺癌组织中Ki-67蛋白的阳性表达率为70.91%(78/110),HIF-1α蛋白的阳性表达率为50.91%(56/110)。不同肿块形态、钙化灶形态、血流显像分级乳腺癌患者乳腺癌组织中Ki-67蛋白阳性表达率比较,差异均有统计学意义(P﹤0.05)。不同血流显像分级乳腺癌患者乳腺癌组织中HIF-1α蛋白阳性表达率比较,差异有统计学意义(P﹤0.05)。结论乳腺癌患者乳腺癌组织中HIF-1α的表达可能与血流显像分级有关,Ki-67的表达可能与肿块形态、钙化灶形态及血流显像分级有关。     

肾母细胞瘤MIB-1（Ki-67增殖指数）和p27kip1表达及与预后的关系

目的:探讨肾母细胞瘤MIB-1（Ki-67增殖指数）和细胞周期蛋白依赖性激酶抑制剂p27kip1的表达及与预后的关系。方法:经医院伦理委员会批准，连续纳入2008年1月至2013年8月在我院就诊的肾母细胞瘤患者样本作为研究对象，观察p27kip1和MIB-1阳性表达与患者临床特征的关系。结果:肿瘤组织中MIB-1阳性表达率高于正常肾组织，p27kip1阳性表达率低于正常肾组织，差异均有统计学意义（P＜0.05）。MIB-1和p27kip1表达与性别、年龄、病理分型、发病部位等均无相关性（P＞0.05），与临床分期存在相关性（P＜0.05）。MIB-1表达阳性患者中位生存时间低于阴性患者，而p27kip1表达阴性患者中位生存时间低于阳性患者（χ2=6.979、15.247，P=0.008、0.000）。结论:MIB-1表达增加和p27kip1表达降低与肾母细胞瘤的发生、发展、预后密切相关，临床应根据其表达情况进行针对性干预，以改善患者的预后。