女性泌尿生殖道支原体感染及耐药性观察

目的了解女性泌尿生殖道感染患者解脲支原体(Uu)和人支原体(Mh)感染及耐药情况,指导临床合理应用抗菌药物。方法采用法国梅里埃公司生产的IST2支原体培养及药敏试剂盒,对932例女性泌尿生殖道感染患者进行培养及药敏试验。结果 932例患者中支原体阳性426例,总检出率45.7%,其中Uu阳性354例(37.9%),Mh阳性14例(1.5%),Uu+Mh阳性58例(6.2%);药敏结果表明,Uu与Mh对多西环素、交沙霉素、四环素较为敏感,Uu对环丙沙星、氧氟沙星耐药率较高,而Mh对克拉霉素、红霉素、阿奇霉素耐药率较高。结论女性泌尿生殖道支原体检出率较高,主要以Uu为主,Uu和Mh对多种抗菌药物耐药,应引起临床重视。     

887例宫颈分泌物支原体培养及耐药性分析

目的 了解女性泌尿生殖道感染患者支原体感染及耐药情况.方法 采用生物梅里埃IST2试剂盒,对887例宫颈分泌物进行培养及药敏试验.结果 887例标本中检出Uu阳性401例(45.2％),Mh阳性4例(0.5％),Uu+Mh阳性137例(15.4％),共检出542例(61.1％).药敏结果表明,Uu与Mh对原始霉素、交沙霉素、强力霉素、四环素较为敏感,对环丙沙星耐药率最高.结论 女性泌尿生殖道Uu和Mh感染率很高,主要以Uu为主,Uu和Mh对多种抗菌药物耐药,其中以环丙沙星为最高,单纯Uu、Mh和Uu+ Mh的耐药率存在一定差异,治疗支原体感染首选交沙霉素、四环素.     

4103例泌尿生殖道支原体感染及药敏分析

目的通过分析泌尿生殖道支原体感染及药敏情况,为临床提供用药指导。方法采用支原体检测试剂盒进行支原体属培养和药敏试验。结果4103例患者标本中,检出支原体属1336株,总阳性率为32．56％;其中单一解脲脲原体（Uu）感染1227例,阳性率为91．84％;单纯人型支原体（Mh）感染15例,阳性率为1．12％;Uu＋Mh混合合感染94例,阳性率为7．04％。解脲脲原体对阿奇霉素、红霉素、交沙霉素、罗红霉素、米诺环素、强力霉素敏感性高;单纯人型支原体对交沙霉素、米诺环素、强力霉素敏感。结论泌尿生殖道支原体感染以Uu为主。支原体大多具有多重耐药性,临床治疗需根据药敏结果选药物。     

女性生殖道支原体感染现状及耐药性调查分析

目的 了解女性生殖道支原体感染现状及耐药性,采取有效措施降低感染率,同时为临床合理用药提供依据.方法 对415例疑似生殖道感染标本采用珠海迪尔生物有限公司生产的试剂盒进行支原体培养和药敏试验.结果 415例女性生殖道标本中,支原体感染209例,阳性率为50.4％(209/415),其中单纯解脲脲原体(Uu)感染141例,阳性率34.0％(141/415),单纯人型支原体(Mh)感染25例,阳性率6.0％ (25/415),Uu和Mh混合感染43例,阳性率为10.4％ (43/415);药敏试验结果表明:Uu、Uu+ Mh、Mh对强力霉素、交沙霉素、美满霉素、四环素敏感性普遍较高,相反对红霉素、环丙沙星、罗红霉素、氧氟沙星等敏感性较差.结论 女性生殖道支原体感染率较高,已婚育龄妇女应加强妇科检查,做到早检查、早诊断、早治疗.同时,临床医生应结合药敏试验结果合理用药,以降低女性生殖道支原体感染的发生率.     

2006～2010年泌尿生殖道炎症患者支原体感染率检测与耐药性分析

目的 了解杭州市萧山区2006～ 2010年泌尿生殖道炎症患者支原体感染及耐药情况.方法 对4 023例泌尿生殖道炎症患者用支原体鉴定及药敏试剂盒进行支原体培养及药敏试验.结果 支原体总检出率为48.1％,女性检出率51.2％明显高于男性41.8％ (P ＜0.05).支原体培养阳性患者中Uu单独感染1701例(88.0％),Mh单独感染57例(2.9％),Uu+ Mh混合感染176例(9.1％),Uu单独感染明显高于Mh单独感染和Uu+ Mh混合感染(P＜0.05).5年间支原体阳性检出率从2006年的39.4％到2010年的58.1％逐年增高,感染模式观察期内无明显变化.支原体对交沙霉素、原始霉素和强力霉素均敏感(敏感率≥91.4％),对四环素、红霉素、氧氟沙星和环丙沙星的耐药率高,均大于50％.比较2006年至2010年各种支原体对9种药物的耐药率,除四环素外耐药率呈不同程度上升,四环素耐药率2007年和2008年较高,后逐年下降,2010年为53.5％.混合感染总体耐药率比Uu或Mh单独感染耐药率高.结论 泌尿生殖道炎症患者支原体感染Uu比较常见,且女性检出率显著高于男性.临床分离支原体大多具有多重耐药性,临床治疗需根据药敏结果加以选择.     

1796例泌尿生殖道支原体培养及药敏结果分析

目的分析新乡地区1796例泌尿生殖道标本的支原体培养及抗生素药物敏感试验,指导临床合理使用抗生素。方法支原体培养鉴定、药敏试剂盒购自贝瑞特公司。同时检测解脲支原体和人型支原体,并进行10种抗生素的药敏试验。数据统计采用χ^2检验。结果支原体培养1596例标本中,541例解脲脲原体（Uu）阳性,阳性率为33.9%;39例人型支原体（Mh）阳性,阳性率为2.4%;解脲脲原体、人型支原体均阳性76例,阳性率为4.8%。200例正常对照组27例阳性,阳性率为13.5%。药敏结果显示,强力霉素、克拉霉素和美满霉素的抗菌活性较强。结论支原体感染以Uu为主,Uu＋Mh次之,正常人泌尿生殖道支原体阳性率为13.5%。只有某些血清型感染且在达到一定浓度以上同时宿主处于多种病原体感染或免疫机制紊乱时,Uu才能致病。避免滥用抗生素引起生殖道菌群失调。临床上治疗Uu感染、Mh感染或Uu＋Mh混合感染时,建议选用强力霉素、克拉霉素和美满霉素。     

1724例女性生殖道支原体感染调查及耐药性分析

目的了解本地区女性生殖道支原体的感染现状及耐药情况,为临床用药提供指导。方法采用生殖道支原体检测试剂盒,对2012年8月至2013年4月解放军第44医院妇科门诊就诊的1 724例女性生殖道标本进行支原体培养及药敏检测,并对结果做统计学分析。结果 1 724例女性生殖道支原体感染率为43.6%,其中单纯Uu感染占85.1%;单纯Mh感染占3.7%;Uu合并Mh感染占11.2%。感染人群中21-40岁年龄段占85.2%。支原体对交沙霉素、强力霉素、美满霉素耐药率较低,对环丙沙星、左氧氟沙星、红霉素及司帕沙星的耐药率较高,单纯Mh及Uu合并Mh感染对抗菌药物的耐药率高于单纯Uu感染。结论女性生殖道支原体感染以单纯Uu为主,感染人群多见于21-40岁,支原体对常用抗菌药物出现了不同程度的耐药性,建议临床根据药敏结果合理用药,以减少耐药菌株的产生。     

2007-2011年杭州市萧山区女性支原体感染及耐药性分析

目的 调查女性泌尿生殖道炎症解脲脲原体(Uu)和人型支原体(Mh)感染及其对抗菌药物耐药性,以了解本地区女性支原体感染状况并指导临床合理使用抗菌药物.方法 采用生物梅里埃Mycoplasma IST支原体鉴定、药敏试剂盒,对女性生殖道感染患者进行支原体培养及药敏试验,所有数据采用WHONET 5.6软件进行回顾性分析.结果 14 894份标本中检出支原体8319例,阳性率55.9％,其中解脲脲原体6 316例(42.4％),人型支原体282例(1.9％),解脲脲原体和人型支原体混合感染1 721例(11.6％).支原体对喹诺酮类耐药率较高(≥39.8％),对多西环素、普拉霉素、四环素和交沙霉素耐药率较低(≤7.0％).结论 Uu是女性泌尿生殖道支原体感染的主要病原体;多西环素、四环素和交沙霉素可作为本地区非淋病性尿道炎(NGU)的首选药物,环丙沙星耐药率出现明显的上升趋势,经验用药避免使用喹诺酮类药物,治疗时应根据药敏结果合理选用抗生素以防止耐药菌株的增加和播散.     

2011—2015年不同年龄段男女患者泌尿生殖道支原体感染状况及耐药性调查

摘要：目的 了解本地区男女患者泌尿生殖道支原体感染状况及耐药特征,为临床诊疗及合理用药提供依据。方法 选取2011年1月—2015年12月门诊及住院患者,采集泌尿生殖道标本做支原体培养,并对阳性标本进行药敏试验,对阳性标本及其药敏结果进行分析。结果 2011年—2015年男女患者的感染率和总感染率呈逐年递增趋势（P＜0.01）,女性感染者高于男性,男女患者均以Uu单纯感染为主,不同年度均以21岁～30岁年龄段患者为主,占合计中51.0%,药敏试验表明Uu+Mh混合感染的耐药率明显高于Uu、Mh单纯感染,Uu+Mh混合感染对克拉霉素、阿奇霉素、罗红霉素、环丙沙星的耐药率均＞90.0%,Uu、Mh和Uu+Mh对美满霉素、强力霉素、交沙霉素的耐药率较低,均＜10.0%。结论 本地区支原体感染呈逐年上升趋势,女性感染率高于男性,年龄21～30岁患者居多,并以Uu单纯感染为主,治疗支原体感染首选美满霉素、强力霉素、交沙霉素。     

非淋菌性泌尿生殖道炎支原体感染及耐药变迁

目的探讨解脲支原体（Uu）及人型支原体（Mh）在非淋菌性泌尿生殖道炎的感染状况,分析近3年来支原体的感染及耐药变迁。方法采用培养法（Mycoplasma IST）对NGGU的分泌物进行支原体的培养、体外药敏试验及分析。结果支原体阳性率为47．0％,其中Uu阳性率为34．0％,Uu＋Mh阳性率为11．4％,Mh阳性率为1．6％;交沙霉素、强力霉素等药物的敏感率无明显变化,而喹诺酮类的耐药率则呈逐渐上升趋势,环丙沙星及氧氟沙星的耐药率分别从2002年的38．9％及40．0％上升到了2004年的79．2％及66．4％。结论支原体的耐药率正逐步增加,其中喹诺酮类的高耐药率提示其在治疗支原体感染中的地位改变,泌尿生殖道支原体的药物敏感监测对临床治疗具有重要意义。     

Race and Racism in America and in Anthropology

Race in North America: Origin and Evolution of a Worldview . Audrey Smedley
Anthropology and Race . Eugenia Shanklin     

Degradation and conversion of somatostatin in normal and diabetic rats in vivo and in vitro

Plasma somatostatin-like immunoreactivity in the portal and jugular veins of streptozotocin diabetic rats was compared with that in normal control rats. In the diabetic group, somatostatin levels in the portal (p less than 0.05) and jugular (p less than 0.01) veins were both elevated compared with those in the control group. Moreover, the degree of elevation was greater in the jugular vein than in the portal vein. To further investigate the role of the liver in the clearance of somatostatin-28 in vivo, 2 micrograms of somatostatin-28 was administered as a bolus into the external jugular vein of intact and functionally hepatectomized rats. The mean half-time of somatostatin-28 was significantly longer in intact diabetic rats than in controls (p less than 0.05). The functional hepatectomy did not cause a significant difference in the half-time in diabetic rats but made it longer in control rats. These results suggest that the longer half-time of somatostatin-28 in diabetic rats in vivo is due to its slower hepatic clearance. The hepatic clearance of somatostatin-28 and somatostatin-14 was further studied in vitro using a recirculating liver perfusion method. The hepatic clearance of 1.2 nM of either somatostatin-28 or somatostatin-14 was significantly lower in diabetic rats than in controls (p less than 0.01). This indicates that elevated plasma somatostatin levels in diabetic rats are caused at least in part by decreased hepatic clearance of somatostatin.(ABSTRACT TRUNCATED AT 250 WORDS)     

MPD and DNA Bending in Crystals and in Solution

Bending of 15 to 24° is observed within crystal structures ofB-DNA duplexes, is strongly sequence-dependent, and exhibits no correlation with the concentration of MPD (2-methyl-2,4-pentanediol) in the crystallizing solution. Two types of bends are observed: facultative bends or flexible hinges at junctions between regions of G·C and A·T base-pairs, and a persistent and almost obligatory bend at the center of the sequence R-G-C-Y. Only A-tracts are characteristically straight and unbent in every crystal structure examined to date. A detailed examination of normal vector plots for individual strands of a double helix provides an explanation, in terms of the stacking properties of guanine and adenine bases. The effect of high MPD concentrations, in both solution and crystal, is to decrease local bending somewhat without removing it altogether. MPD gel retardation experiments provide no basis for choosing among the three models that seek to explain macroscopic curvature of DNA by means of microscopic bending: junction bending, bent A-tracts, or bent general- sequence DNA. Crystallographic data on the straightness of A-tracts, the bendability of non-A sequences, and the identity of inclination angles in A-tract and non-A-tractB-DNA support only the general-sequence bending model. The pre-melting transition observed in A-tract DNA probably represents a relaxation of stiff adenine stacks to a flexible conformation more typical of general-sequence DNA.     

Deoxynivalenol and nivalenol in wheat and by-products in Argentina

The deoxynivalenol and nivalenol contamination in wheat and by-products obtained through milling was analized by Trucksess method slightly modified in the proportion of acetonitrile—water (3:1). Only one sample of wheat showed deoxynivalenol contamination, 1,200μg/kg. No samples obtained in different stages of the milling were contaminated with deoxynivalenol or nivalenol. In the commercial wheat flours the levels found ranged between 400 and 800μg/kg, as follows: 400μ/kg, 5 samples; 800jug/kg, 1 sample.     

Obestatin and ghrelin in obese and in pregnant women

We identified, through qPCR, receptor mRNA for a number of gut peptides in female human omental fat: the incretins, GIP and GLP-1, the orexigenic peptides PYY-Y1 and -Y2 and ghrelin, and the anorexigenic peptide obestatin. Four cohorts of women were examined: lean controls (BMI<23), obese (BMI>41), obese diabetic and term pregnant women. Human fat expressed receptor mRNAs for all six peptides. Pregnant women expressed roughly three times as much orphan GPR-39 receptor, a proposed obestatin receptor, than other women and less than half as much of the ghrelin receptor (GHSR-1a). An immunoblot probed with a GPR-39 selective antibody yielded a single band corresponding to the correct molecular weight (52 kDa) for the proposed obestatin receptor. Fluorescent immunohistochemistry of human fat employing the same antibody indicated the receptor protein was localized to the adipocyte cell membrane. The concentration of obestatin circulating in blood was measured in the same cohort of women and was significantly lower in obese and obese diabetic women compared to control.