袖状胃切除术对甲状腺功能正常的肥胖患者甲状腺功能的影响

目的观察腹腔镜下袖状胃切除术(laparoscpic sleeve gastrectomy, LSG)对甲状腺功能正常的肥胖患者甲状腺功能的影响。方法纳入2012年12月—2018年5月在同济大学附属第十人民医院进行LSG手术的甲状腺功能正常的51名肥胖患者为研究对象,以促甲状腺激素(thyroid stimulating hormone, TSH)=2.5 mIU/L为切点,将其分为正常TSH组(A组: 0.38~2.5 mIU/L)和高TSH组(B组: 2.5~4.34 mIU/L)。收集两组LSG术前、术后6个月的身高、体质量、甲状腺功能相关数据;采用双能X线吸收法测定身体各部位脂肪含量。结果 LSG术后6个月A组TSH降低无统计学意义( P =0.855),而B组TSH降低有统计学意义(P<0.05)。Pearson相关分析结果显示,女性和B组肥胖患者ΔTSH与ΔBMI、总体质量减少百分比以及多余体质量减少百分比呈显著的正相关(均0< r <1, P <0.05)。将Pearson相关分析中与ΔTSH相关的变量以及可能影响ΔTSH的相关因素代入多因素线性回归模型,结果显示年龄、ΔAndroid和ΔBMI是影响ΔTSH的独立危险因素。结论 LSG可以降低术前TSH在2.5~4.34 mIU/L的肥胖患者的TSH水平,而对于术前TSH在0.38~2.5 mIU/L的肥胖患者的TSH无明显作用。年龄、术后BMI和Android部位脂肪含量的变化是预测甲状腺功能正常的肥胖患者术后TSH变化的重要因素。

甲状腺癌诊治的多学科协作诊疗策略

甲状腺癌的发病率在我国呈明显上升趋势,但在治疗过程中存在很大的随意性和不规范性,并且甲状腺良性结节的过度治疗比例高。多学科专家组诊疗(multidisciplinary team,MDT)模式已成为肿瘤治疗的模式和发展方向。上海市甲状腺疾病研究中心的建立是对MDT模式的进一步探索和优化。文章结合本中心的临床诊疗流程和经验,探讨甲状腺癌MDT及一体化诊疗的优势及意义,为推广此模式和规范治疗提供参考。

真实世界甲状腺癌的诊疗现状与思考

随着全球性的甲状腺癌发病率的不断增加,甲状腺癌的诊疗规范引起更多的关注和争议。真实世界诊疗现状与诊疗原则的差异也是影响发病率和预后的重要因素。文章从真实世界的临床诊疗现状出发,提出临床问题,给出临床建议,并探讨进一步建立以疾病为中心的个体化治疗,为以科学为导向的诊疗规范提供参考。

Liraglutide prevents high glucose level induced insulinoma cells apoptosis by targeting autophagy

Background The pathophysiology of type 2 diabetes is progressive pancreatic beta cell failure with consequential reduced insulin secretion. Glucotoxicity results in the reduction of beta cell mass in type 2 diabetes by inducing apoptosis. Autophagy is essential for the maintenance of normal islet architecture and plays a crucial role in maintaining the intracellular insulin content by accelerating the insulin degradation rate in beta cells. Recently more attention has been paid to the effect of autophagy in type 2 diabetes. The regulatory pathway of autophagy in controlling pancreatic beta cells is still not clear. The aim of our study was to evaluate whether liraglutide can inhibit apoptosis and modulate autophagy in vitro in insulinoma cells （INS-1 cells）. Methods INS-1 cells were incubated for 24 hours in the presence or absence of high levels of glucose, liraglutide （a long-acting human glucagon-like peptide-1 analogue）, or 3-methyadenine （3-MA）. Cell viability was measured using the Cell Counting Kit-8 （CCK8） viability assay. Autophagy of INS-1 cells was tested by monodansylcadaverine （MDC） staining, an autophagy fluorescent compound used for the labeling of autophagic vacuoles, and by Western blotting of microtubule-associated protein I light chain 3 （LC3）, a biochemical markers of autophagic initiation. Results The viability of INS-1 cells was reduced after treatment with high levels of glucose. The viability of INS-1 cells was reduced and apoptosis was increased when autophagy was inhibited. The viability of INS-1 cells was significantly increased by adding liraglutide to supplement high glucose level medium compared with the cells treated with high glucose levels alone. Conclusions Apoptosis and autophagy were increased in rat INS-1 cells when treated with high level of glucose, and the viability of INS-1 cells was significantly reduced by inhibiting autophagy. Liraglutide protected INS-1 cells from high glucose level-induced apoptosis that is accompanied by a significant increase of autophagy, suggesting that liraglutide plays a role in beta cell apoptosis by targeting autophagy. Thus, autophagy may be a new target for the prevention or treatment of diabetes.