API2-MALT1融合基因变异体在粘膜相关淋巴组织结外边缘区B细胞淋巴瘤中的分布及凋亡的关系

目的探讨API2-MALT1融合基因变异体在粘膜相关淋巴组织结外边缘区B细胞淋巴瘤(extranodal marginal zone B—cell lymphoma of mucosa—associated lymphoid tissue，MALT)中的分布特点及其转录与肿瘤凋亡的关系。方法将逆转录-聚合酶链反应和巢式聚合酶链式反应结合，检测62例不同部位MALT淋巴瘤中API2-MALT1融合基因的多种变异体；通过TdT介导脱氧核苷酸缺口末端标记技术进行肿瘤细胞的原位凋亡检测；通过逆转录-聚合酶链反应和免疫组化染色检测API2的mRNA和蛋白水平。结果62例MALT淋巴瘤中28例检出API2-MALT1融合基因(45．16％)，为变异体A1446-M1123或A1446-M814，但未检出A1446-M541和A1446-M1150。A1446-M1123(18／28)的检出明显多于A1446-M814(10／28)。融和基因转录在甲状腺MALT淋巴瘤中检出最低，在其它部位的分布无差异。在API2-MALT1^ 组(API2-MALT1mRNA表达阳性组)肿瘤凋亡水平明显高于API2-MALT1^-组(API2-MALT1mRNA表达阴性组)，API2的mRNA和蛋白水平低于阴性组。A1446-M1123^ 与A1446-M814^ 病例之间凋亡和API2的变化无差异。结论MALT淋巴瘤中t(11；18)(q21；q21)的发生有部位差异，A1446-M1123可能是中国人MALT淋巴瘤中API2-MALT1融合基因变异体的主要类型。API2-MALT1融合基因转录与MALT淋巴瘤的凋亡水平和API2的变化有关。     

API0134对血小板α颗粒膜蛋白和血小板聚集的影响

２０例急性心肌梗死患者在溶栓后随机分为穿心莲有效成分（ＡＰＩ０１３４,ＡＰＩ）组与对照组,治疗１５ｄ,均同时给予阿司匹林等药物。检测溶栓前后血浆α颗粒膜蛋白（ＧＭＰ－１４０）浓度和ＡＤＰ诱导的血小板聚集反应。结果表明,ＡＰＩ组溶栓后７２ｈ血浆ＧＭＰ－１４０浓度轻度增加,对照组显著性增加（Ｐ＜０．０１）。ＡＰＩ组ＧＭＰ－１４０在溶栓后７２ｈ和１５ｄ均低于对照组,差异有显著意义（均为Ｐ＜０．０５）。ＡＰＩ组１ｍｉｎ和５ｍｉｎ血小板聚集率均低于对照组,差异均有显著意义（７２ｈ,Ｐ＜０．０５;１５ｄ,Ｐ＜０．０１）。研究表明,ＡＰＩ与阿司匹林联合应用可抑制溶栓后血小板的活化,优于阿司匹林单独应用,因此ＡＰＩ有可能用于临床预防溶栓后的再闭塞。     

API在一次生物性突发公共卫生事件鉴定中的应用

法国梅里埃API始创于1970年，是一系列微生物鉴定用试剂盒。法国梅里埃API的使用使细菌鉴定更简单、快速和可靠。随着被微生物学家的广泛应用，法国梅里埃API系列已成为国际上公认的鉴定细菌的参考标准。     

Phoenix-100全自动微生物鉴定/药敏系统检测肠球菌方法评估

目的用Phoen ix-100全自动微生物鉴定/药敏系统(简称Phoen ix-100系统)检测肠球菌并评估此检测系统。方法收集50株临床分离肠球菌,用Phoen ix-100系统进行鉴定及药敏试验,通过与API鉴定系统、药敏纸片法和E-test法[筛选耐万古霉素肠球菌(VRE)]比较,对Phoen ix-100系统进行评估。结果与API鉴定系统相比,Phoen ix-100系统鉴定肠球菌的一致率为90.0%。与药敏纸片法相比,Phoen ix-100系统检测肠球菌对庆大霉素(筛选耐高浓度氨基糖苷类抗生素肠球菌)、氨苄西林、环丙沙星、红霉素、呋喃妥因、万古霉素和肽可霉素药敏结果的完全符合率分别为94.0%、94.0%、88.0%、94.0%、70.8%、64.0%和92.0%。与E-test法相比,Phoen ix-100系统筛选VRE的完全符合率为84.0%;未出现极大错误,大错误率为12.0%,小错误率为4.0%。结论用Phoen ix-100系统检测肠球菌是一种简便、快速和比较准确可靠的方法。     

广东省香港海鸥菌感染性腹泻1例分析

目的了解广东省获得性胃肠炎患者中是否存在香港海鸥型菌(LH)感染。方法2009年4月～12月选择江门市各级医院门诊腹泻患者,采集肛拭子标本,培养分离可疑菌株,经革兰染色、生化鉴定、特异性片段PCR扩增和16S rRNA基因序列测定,进行香港海鸥型菌的鉴定。结果在804例腹泻患者标本中,分离并鉴定1株香港海鸥型菌,符合已有报道菌的菌落特点和生化特征,命名为江门株(JM1),16S rRNA目的基因扩增长度为426 bp,基因序列长度为1 360 bp,与香港分离菌株(NR-025167)同源性为99%,确诊为香港海鸥型菌感染病例。结论证实广东省内社区获得性胃肠炎患者中存在香港海鸥型菌的感染。     

INSECTICIDE-TREATED BED NETS IN ROND?NIA,BRAZIL: EVALUATION OF THEIR IMPACT ON MALARIA CONTROL

Mosquito nets treated with long-lasting insecticide (LLINs), when used in compliance with guidelines of the World Health Organization, may be effective for malaria vector control. In 2012, approximately 150,000 LLINs were installed in nine municipalities in the state of Rondônia. However, no studies have assessed their impact on the reduction of malaria incidence. This study analyzed secondary data of malaria incidence, in order to assess the impact of LLINs on the annual parasite incidence (API). The results showed no statistically significant differences in API one year after LLIN installation when compared to municipalities without LLINs. The adoption of measures for malaria vector control should be associated with epidemiological studies and evaluations of their use and efficiency, with the aim of offering convincing advantages that justify their implementation and limit malaria infection in the Amazon Region.     

原料药中基因毒性杂质控制的研究进展

目的介绍原料药(active pharmaceutical ingredient,API)中基因毒性杂质控制的法规要求、评估方法和控制方法。方法通过学习欧美法规发展历史,理解国际高端市场对基因毒性杂质控制的监管期望,提出原料药中基因毒性杂质风险评估方法。结果与结论企业基于半定量评估,结合清除研究数据,建立科学的控制策略,使实际工艺中所有可能涉及的基因毒性杂质风险得到明确鉴别和控制,是达到监管期望的有效途径。     

Sensitivity pattern of gram negative bacilli to three beta-lactam/beta-lactamase inhibitor combinations using the automated API system

PURPOSE: To evaluate the spectrum of activity of three beta-lactamase inhibitors such as amoxicillin/ clavulanic acid, ticarcillin/ clavulanic acid and piperacillin/ tazobactam in comparison to cephalosporins against gram negative bacilli. METHODS: Gram-negative bacilli isolated from the clinical specimens received in the laboratory were included in the study. Using the API system (bioMiotarieux) during a one-year period, a total of 1,252 Enterobacteriaceae and 385 non-fermenters were evaluated. RESULTS: The percentage resistance of the Enterobacteriaceae isolates was 82.92% to amoxicillin/ clavulanic acid, 58.22% to ticarcillin/clavulanic acid and 22.44% to piperacillin/tazobactam respectively. Pseudomonas aeruginosa showed resistance of 96% to ticarcillin/ clavulanic acid and 61% to piperacillin/ tazobactam and Acinetobacter baumannii showed 49% resistance to ticarcillin/ clavulanic acid and 77% resistance to piperacillin/ tazobactam respectively. The isolates exhibited high resistance to all the generations of cephalosporins and the other groups of antibiotics except carbapenems. CONCLUSIONS: Piperacillin/tazobactam was found to be the most active combination of the three against Enterobacteriaceae and Pseudomonas spp. and ticarcillin/clavulanic acid against Acinetobacter spp. and Stenotrophomonas maltophilia.     

The Selection of a Pharmaceutical Salt—The Effect of the Acidity of the Counterion on Its Solubility and Potential Biopharmaceutical Performance

A roadmap for the selection of a pharmaceutical salt form for a development candidate is presented. The free base of the candidate did not have sufficient chemical stability for development. The initially selected salt form turned out to be undevelopable because it was unstable during scale-up synthesis and storage. The rationale for the new solid form screening and the criteria for selection are discussed. Before the final selection, the pH solubility profiles of the 2 new salts, a benzoate and a besylate, were compared. Atypical solubility behavior was observed for the benzoate salt in hydrochloric acid with and without normal saline. A scheme is proposed illustrating how the pKas of the counterion and active pharmaceutical ingredient, the medium composition, and final pH affect the solubility and solution equilibria of the 2 selected salt forms. This scheme also includes the equilibria between solution and solid phases in different pH ranges. The pharmaceutical importance of this research is that it sheds light on how the acidity of the counterion can affect the solubility of the selected salt form in the gastric environment. With a well-designed formulation strategy, this property potentially can be translated to optimal biopharmaceutical performance of the drug product.