The Role of Pyridoxine in the Prevention and Treatment of Neuropathy and Neurotoxicity Associated with Rifampicin-Resistant Tuberculosis Treatment Regimens: A Topic Review

Rifampicin-resistant tuberculosis (RR-TB) is a global public health problem caused by mycobacterium tuberculosis resistant to Rifampicin. Drug-induced peripheral neuropathy and neurotoxicity are well-known adverse effects of treatment regimens that cause significant morbidity. Pyridoxine is often added to treatment regimens for the prevention and/or treatment of these side effects. The basis and effectiveness of this practice are unclear. We conducted a systematic review to evaluate the effectiveness of pyridoxine in preventing and/or treating neuropathy and neurotoxicity associated with RR-TB treatment. We included studies with patients with RR-TB who experienced neuropathy or neurotoxicity attributed to RR-TB regimens and were given pyridoxine. Our findings showed contradicting evidence on the use of pyridoxine for preventing or treating neurotoxicity due to cycloserine in the treatment of RR-TB. Moreover, pyridoxine did not have a protective effect against neuropathy and/or neurotoxicity caused by other RR-TB regimens that do not contain isoniazid. In conclusion, we found that withdrawing or withholding medications such as linezolid, cycloserine, thioamides, fluoroquinolones, and ethambutol, implicated in causing neuropathy or neurotoxicity was more effective than using pyridoxine to stop the progression of symptoms, and in some instances, led to their reversal over time.

Resistant Pulmonary TB-HIV Co-Infection in an Infant: About a Case

Diagnosis of childhood tuberculosis (TB) is difficult, especially in resource-limited countries where the number of reported cases of TB-HIV co-infection continues to rise. This co-infection poses a diagnostic and therapeutic problem for caregivers. We report a case of rifampicin-resistant HIV-TB pulmonary coinfection in a 19-month-old infant.

Luciferase reporter phage phAE85 for rapid detection of rifampicin resistance in clinical isolates of Mycobacterium tuberculosis

Objective:To evaluate luciferase reporter phage(LRP)phAE85 in rapid detection of rifampicin resistance in a region where TB is endemic.Methods:One hundred and ninety primary isolates on Lowenstein-Jensen medium were tested.Middlebrook 7H9 complete medium with and without rifampicin at 2μg/mL was inoculated with standard inoculum from suspensions of the clinical isolate.After incubation for 72 h,LRP was added.Following 4 h of further incubation,light output from both control and test was measured as relative light units.Strains exhibiting a reduction of less than 50%relative light units in the drug containing vial compared to control were classified as resistant.Results were compared with the conventional minimum inhibitory concentration method(MIC)of drug susceptibility testing.Results:The two methods showed high level of agreement of 97%(CI 0.94,0.99)and P value was 0.000 1.The sensitivity and specificity of LRP assay for detection of rifampicin resistance were 91%h(CI 0.75,0.98)and 99ct(CI0.95,1.00)respectively.Time to detection of resistance by LRP assay was 3 d in comparison with 28 d by the minimum inhibitory concentration method.Conclusions:LRP assay with phAE85 is 99%specific,91%sensitive and is highly reproducible.Thus the assay offers a simple procedure for drug sensitivity testing,within die scope of semi-automation.

Low Doses of Rifampicin Used in New Tuberculosis Patients Correlated to Increased Frequency of Rifampicin-Resistance and Poorer Treatment Outcomes

The prognosis of patients with previously treated tuberculosis (TB) was suggested to be dependent on whether the initial treatment was in compliance with the established guidelines. The aim of this retrospective multicenter study was to determine the proportion of new TB patients who received standard doses of rifampicin in multiple provinces of China, and the relationship between low doses of rifampicin and frequency of rifampicin-resistance as well as treatment outcomes. A total of 713 new TB patients were treated with either once-daily dose of bulk anti-TB drugs (group I) or every other day combination blister packs of anti-TB drugs containing rifampicin (group II) at more than 30 TB treatment centers/hospitals in China. Treatment history, therapeutic doses of rifampicin, and information about patients were extracted from their medical records and analyzed, and rifampicin-resistance of isolates collected from patients following the treatment as well as treatment outcomes were compared between two treatment groups. Among 522 patients in treatment group I, 154 (29.5%) received standard and 363 (69.5%) received low doses of rifampicin;238 (45.6%) isolates were rifampicin-resistant, and 243 (46.6%) were successfully treated. Among 191 patients in treatment group II, 175 (91.6%) received standard and 15 (7.9%) received low doses of rifampicin;72 (37.7%) isolates were rifampicin-resistant, and 105 (55%) were successfully treated. When patients who received low doses of rifampicin were compared to others within the same treatment group, increased rates for rifampicin-resistance and treatment failure were observed. Results from this study showed that most new TB patients in treatment group I (69.5%) received low doses of rifampicin, and their treatment outcomes were worse than those in treatment group II, indicating that low doses of rifampicin used for the initial treatment of new TB patients were correlated to increased frequency of rifampicin-resistance and poorer treatment outcomes.

Multidrug-Resistant Tuberculosis in the Democratic Republic of Congo: Analysis of Continuous Surveillance Data from 2007 to 2016

Background: For countries with limited resources such as the Democratic Republic of the Congo (DRC), the diagnosis of Multidrug-resistant tuberculosis (MDR-TB) is still insufficient. The MDR-TB identification is done primarily among at-risk groups. The knowledge of the true extent of the MDR-TB remains a major challenge. This study tries to determine the proportion of MDR-TB in each group of presumptive MDR-TB patients and to identify some associated factors. Methods: This is an analysis of the DRC surveillance between 2007 and 2016. The proportions were expressed in Percentage. The logistic regression permits to identify the associated factors with the RR-/MDR-TB with adjusted Odds-ratio and 95% CI. Significance defined as p ≤ 0.05. Results: Overall, 83% (5407/6512) of the MDR-TB presumptive cases had each a TB test. 86.5% (4676/5407) had each a culture and drug sensitive testing (DST) on solid medium, and 24.3% (1312/5407) had performed an Xpert MTB/RIF test. The proportion of those with at least one first-line drug resistance was 59.3% [95% CI 57.2 - 61.4] among which 50.1%, [95% CI 47.9 - 52.3] for the isoniazid, 45.6% [95% CI 43.4 - 47.8] for the rifampicin, 49.9% [95% CI 47.8 - 52.1] for ethambutol and 35.8% [95% CI 33.7 - 37.9] for streptomycin. The confirmation of MDR-TB was 42.8% [95% CI 38.4 - 47.8]. Combining both tests, the proportion of RR-/MDR-TB was 49.6% [95% CI 47.9 - 51.4] for all presumptives. This proportion was 60.0% for failures, 40.7% for relapses and 34.7% for defaulters. Associated factors with the diagnosis of MDR-TB were: aged less than 35 years;prior treatment failure;defaulters;the delay between the collection of sputum and the test completion. Conclusion: The proportion of RR-/MDR-TB among the presumptives has been higher than those estimated generally. The National tuberculosis programme (NTP) should improve patient follow-up to reduce TB treatment failures and defaulting. Moreover, while increasing the use of molecular tests, they should reduce sample delivery times when they use culture and DST concomitantly.

Prevalence of Multidrug Resistant <i>Mycobacterium tuberculosis</i>among Tuberculosis Patients Admitted to Adama Hospital Medical College, Adama, Ethiopia: A Retrospective Study

Multidrug resistant tuberculosis (MDR-TB) is an emerging challenge for TB control programs globally. Ethiopia ranks 7th among the world’s 22 high TB burden countries. According to report of WHO (2017), TB is one of the leading infectious causes of death in Ethiopia claiming the life of more than 30 thousand people annually. The surge of MDR-TB has been compounding the problem further. Facility-based MDR-TB researches have not been generated in equal pace with community-based ones. The aim of this study was to assess the prevalence of MDR-TB using clinical records of MDR-TB patients in Adama Hospital Medical College (AHMC) from 2014 to 2018. All clinical data of MDR-TB from 2014-2018 was collected from AHMC TB department. Socio-demographic and risk factor data were collected from patients using semi-structured questionnaire. Data were analyzed using Microsoft excel and SPSS version 20. Out of a total 2332 TB suspected cases admitted to AHMC from 2014 to 2018, 175 (7.5%) were confirmed MDR-TB cases or confirmed Rifampicin resistant cases. In particular, 97 (4.2%) presented presumptive MDR-TB alone and 78 (3.3%) showed confirmed Rifampicin resistance alone. Comparison among age groups showed the highest prevalence for 24 - 44 years with 1.8% and 1.5% confirmed MDR-TB and Rifampicin resistance. The overall prevalence of MDR-TB was moderate indicating for possible rise of the problem due to course of time. Further study combining both community and health facility based is recommended to highlight the need to make useful strategies for testing, surveillance and effective clinical management of MDR-TB cases.

Prevalence of Mycobacterium tuberculosis Strains Isolated from Both Pulmonary and Extra Pulmonary Samples and Their Resistance to Rifampicin: A Study from Kolkata and Surrounding Suburbs

Tuberculosis (TB) is one of the major causes of morbidity and mortality worldwide. In India, nearly 1.8 million new cases of TB are reported annually, which accounts for a fifth of new cases in the world—greater than in any other country. Anti-tubercular drugs (ATDs) have been used for decades, and widespread resistance to them is a very serious public health concern in any part of the world. Aim of this study was to determine the prevalence of Rifampicin (the first line Anti-TB drug) resistance among both pulmonary and extra-pulmonary samples tested positive for Mycobacterium tuberculosis and thereby predict the prevalence of Multi-drug resistant (MDR) tuberculosis in Kolkata and its Suburban regions. All 331 randomly collected clinical samples (both Pulmonary and Extra Pulmonary) were initially screened by Zeihl-Neelsen AFB staining followed by culture on BacT/Alert 3D system and on Lowenstein-Jensen medium and the positive samples were subjected to detection of Mycobacterium tuberculosis complex (MTBC) and simultaneous analysis of Rifampicin resistance by Xpert MTB/RIF assay. Out of the 51 (15.40%) culture positive samples, 13.7% of pulmonary samples and 9.09% of extra-pulmonary samples were Rifampicin resistant. The prevalence of Rifampicin resistant TB in our study is high and the possible reasons can be mixing of new as well as retreatment cases and smaller sample size but, yet it can help Government and public health regulatory bodies to formulate adequate strategies to fight against drug resistant tuberculosis, especially in this part of the world.

Rapid Molecular Detection of Tuberculosis and Rifampicine Resistance in Ecuador

Background: In Ecuador, tuberculosis (TB) remains a serious problem that is complicated by the emergence of multidrug-resistant TB (MDR-TB). To evaluate this problem, this study was carried out at the Social Security Hospital (IESS) in Guayaquil, Ecuador from 2013 to 2015. Methods: The Xpert TB/RIF system was used to detect TB and MDR-TB and a survey was carried out to identify the factors that are potentially causing MDR-TB. Findings: 200 TB patients were confirmed on 5649 suspected patients and 20 (10%) with MDR-TB. It was observed that the annual prevalence of TB and MDR-TB had declining during study period. Trends have been declining but co-infection has doubled since 2009 with 16% of patients co-infected with HIV. Potential resistance factors identified were: disruption in drug supply, lack of resources and lack of credibility of treatment.

世界卫生组织对BPaLM方案治疗耐多药结核病指南的解读

耐多药结核病仍是人类健康的重大危险因素,近期世界卫生组织推荐贝达喹啉(bedaquiline,Bdq)、普托马尼(pretomanid,Pa)、利奈唑胺(linezolid,Lzd)和莫西沙星(moxifloxacin,Mfx)的6个月方案(BPaLM)治疗耐多药结核病。新指南中短程方案适用人群扩大到耐多药结核病患者,而且适用于病变广泛的肺结核和大多数肺外结核,无疑是耐多药结核病治疗的重要事件。本文就BPaLM方案的研究历程、适用人群和注意事项作一简要介绍。

广州市“十二五”与“十三五”期间利福平耐药肺结核患者发现与治疗情况分析

目的:分析广州市“十二五”与“十三五”结核病防治规划期间利福平耐药肺结核(RR-PTB)患者发现与治疗情况,为进一步制定本地区RR-PTB防治规划提供科学依据。方法:通过“中国疾病预防控制信息系统”子系统“结核病信息管理系统”,按照登记时间导出2011年1月1日至2020年12月31日,即“十二五”(2011—2015年)和“十三五”(2016—2020年)规划期间广州市登记的肺结核患者耐药病案数据(包括性别、年龄、民族、职业、户籍、耐药类型、治疗分类等相关信息),筛选出利福平耐药患者病案,分析患者登记、人群特征、耐药筛查和治疗转归情况。结果:2011—2020年,RR-PTB患者年均登记率为0.71/10万(1152/16286.08万),从2011年的0.31/10万(42/1346.32万)上升至2015年的0.38/10万(60/1594.95万)和2020年的0.97/10万(182/1874.03万),呈逐年上升趋势(χ_(趋势)^(2)=256.395,P<0.001)。其中,“十二五”期间年均登记率为0.34/10万(250/7358.06万),不同年份登记率的差异无统计学意义(χ_(趋势)^(2)=4.674,P=0.322);“十三五”期间年均登记率为1.01/10万(902/8928.02万),不同年份登记率的差异有统计学意义(χ_(趋势)^(2)=38.439,P<0.001)。1152例患者中,以男性(851例,73.87%)、25~34岁青壮年(257例,22.31%)和家政家务及待业(364例,31.60%)为主;流动人口、初治、RR-PTB(除异烟肼耐药)、广泛耐药肺结核比例分别从“十二五”的8.80%(22/250)、11.20%(28/250)、0.00%(0/250)和0.00%(0/250)上升到“十三五”的54.43%(491/902)、37.14%(335/902)、19.84%(179/902)和0.78%(7/902),差异均有统计学意义(χ^(2)=91.370、298.740、97.915、34.096,P值均<0.001)。广州市耐药肺结核高危人群筛查率由2017年的60.91%(148/243)上升至2020年的98.95%(568/574),新发/初治病原学阳性肺结核耐药应筛查率由2018年的83.93%(1410/1680)提高到2020年的94.99%(3222/3392),差异均有统计学意义(χ_(趋势)^(2)=425.043、269.670,P值均<0.001)。纳入治疗、完成治疗和治疗成功的患者比例分别从“十二五”的81.20%(203/250)、2.46%(5/203)和45.81%(93/203)提高到“十三五”的91.02%(821/902)、33.62%(276/821)和67.48%(554/821),治疗失败患者比例从17.73%(36/203)降低至2.68%(22/821),差异均有统计学意义(χ^(2)=19.112、86.809、46.636、58.572,P值均<0.001)。结论:在“十二五”与“十三五”规划期间,广州市RR-PTB的防治工作取得了显著的成效。下一步工作中需继续坚持政府主导、多部门合作和全社会共同参与的原则,切实落实结核病防治规划要求,加强结核病防治服务体系建设。

Xpert结核分枝杆菌及利福平耐药菌检测在结核病诊断中的应用价值

目的 探讨运用Xpert结核分枝杆菌及利福平耐药菌检测(MTB/RIF)对疑似肺结核患者的诊断效能。方法 结合病原学、影像学诊断结果,选取郑州人民医院和郑州市中心医院2021年1—12月收治的248例疑似肺结核患者为研究对象,留取痰液或肺泡灌洗液进行培养、Xpert MTB/RIF、抗酸染色和液基集菌涂片染色检测,对Xpert MTB/RIF在肺结核疑似患者中的诊断效能进行评估。结果 248例研究对象中,最终诊断为肺结核122例。MTB液体培养、Xpert MTB/RIF、抗酸染色涂片、液基集菌染色检测诊断肺结核的敏感度分别为54.10%、97.54%、7.38%、16.39%,特异度分别为98.41%、98.41%、95.24%、93.65%。Xpert MTB/RIF检测结果的敏感度优于其他3种检测方法,且漏检率最低。结论 Xpert MTB/RIF能提高MTB的阳性检出率,对结核病的早期诊断及有效防控均有益处,具有实际临床应用价值。

54例复治利福平耐药结核病患者菌株遗传特征及耐多药基因分析

目的 分析54例复治利福平耐药结核病(RR-TB)患者的结核分枝杆菌(MTB)菌株遗传特征及耐多药基因突变情况。方法 选择同时留存有初治及复治MTB菌株的复治RR-TB患者54例,取其初治及复治时的MTB共54对(108株),采用RD105基因缺失法检测其基因型,15位点可变数目串联重复序列基因分型实验(MIRU-VNTR)判断其复治发病原因;取复治时的MTB 54株,通过MIRU-VNTR结果构建最小生成树(MST),分析群体遗传特征;采用分子线性探针药敏实验分析复治MTB的耐多药基因(利福平耐药rpo B基因及异烟肼耐药kat G、inh A基因)突变情况。结果 108株复治RR-TB患者的MTB均为北京基因型,内源性复燃占比77.8%(42/54)、外源性再感染占比22.2%(12/54)。MST显示,54株复治MTB分为3个克隆复合群(CC1、CC2、CC3)和13个独特基因型;共48种基因型,成簇率为11.1%。分子线性探针药敏试验结果显示,异烟肼耐药kat G、inh A基因突变40株,耐多药率为74.1%(40/54);利福平耐药rpo B基因以S531L位点突变为主(63.0%,34/54),异烟肼耐药kat G基因以S315T1位点突变为主(75.0%,30/40)。结论 北京地区复治RR-TB患者发病原因主要是内源性复燃,主要流行菌株为北京基因型,呈现出较高的遗传多样性,成簇率较低,MTB耐多药基因突变位点多为rpo B基因S531L及kat G基因S315T1。

不同技术检测利福平耐药预测耐多药结核病的可靠性分析

目的:分析不同技术检测利福平耐药(RR)预测耐多药(MDR)结核病的可靠性。方法:采用回顾性研究方法,从河南省胸科医院“医院信息管理系统”中搜集2021年7月至2022年11月收治的130例开展过MassARRAY核酸质谱技术检测结核分枝杆菌耐药性项目,并获得结核分枝杆菌核酸阳性结果及药物敏感性试验(简称“药敏试验”)数据的结核病患者实验室相关数据,追踪所有患者同期开展的GeneXpert MTB/RIF(简称“Xpert”)和表型药敏试验(pDST)检测结果进行对比分析。结果:在130例MassARRAY检测阳性的结核病患者中,37例(28.46%)报告为RR;102例Xpert检测阳性患者中,38例(37.25%)诊断为RR;48例培养阳性后行pDST的患者中,22例(45.83%)检出RR。在MassARRAY检出RR患者中,MassARRAY和pDST诊断的MDR占比分别为83.78%(31/37)和90.48%(19/21);在Xpert检出RR患者中,MassARRAY和pDST诊断的MDR占比分别为73.68%(28/38)和76.00%(19/25);在pDST检出RR患者中,MassARRAY和pDST诊断的MDR占比分别为90.91%(20/22)和95.23%(20/21);在MassARRAY和Xpert同时诊断RR患者中,MassARRAY和pDST诊断的MDR占比分别为88.89%(24/27)和88.89%(16/18);在MassARRAY或Xpert任一检出RR患者中,MassARRAY和pDST诊断的MDR占比分别为72.92%(35/48)和75.00%(21/28)。结论:不同方法检出RR作为预测MDR的标志具有良好的可靠性,但可靠程度与RR诊断技术的准确性相关。

平顶山地区某医院195例肺结核患者利福平耐药发生与危险因素分析

目的探究平顶山地区某医院195例肺结核患者利福平耐药发生与危险因素。方法回顾性选取我院2019年8月至2023年4月期间收治的650例阳性肺结核患者作为研究对象,分析患者利福平耐药情况,并根据是否利福平耐药分为对照组(利福平敏感,455例)、观察组(利福平耐药,195例),通过单因素及多因素分析法分析肺结核患者利福平耐药的危险因素。结果650例肺结核患者痰标本中分离出650株结核分枝杆菌,其中有195例利福平耐药患者,利福平耐药率为30.00%。多因素Logistic分析结果显示,有合并症、抗结核治疗次数≥2次、自服药物、未按剂量服药、中断治疗、未知晓肺结核的传播途径为肺结核患者利福平耐药的危险因素(OR=9.767、7.471、5.463、6.693、11.056、10.268,P均<0.05)。结论肺结核患者利福平耐药率为30.00%,有合并症、抗结核治疗次数≥2次、自服药物、未按剂量服药、中断治疗、未知晓肺结核的传播途径为肺结核患者利福平耐药的危险因素,临床可据此给予患者针对性治疗及干预措施,以降低肺结核患者利福平耐药的风险。

2018-2022年重庆市复治肺结核患者利福平耐药情况及影响因素

目的分析重庆市复治肺结核患者利福平耐药情况及影响因素,为该市耐药结核病防控工作提供依据。方法应用描述性流行病学方法分析2018—2022年重庆市区县登记的复治肺结核患者利福平耐药情况,采用χ^(2)检验及二元logistic回归分析复治肺结核患者耐药影响因素。结果2018—2022年该市区县复治肺结核患者利福平耐药检出率14.45%(558/3862),总体呈下降趋势(χ_(趋势)^(2)=22.739,P<0.001)。单因素分析显示复治肺结核患者中流动人口、居住在主城都市区、工人及民工患者利福平耐药检出率最高(均P<0.05),随年龄增加利福平耐药检出率降低(P趋势<0.001)。多因素logistic回归分析显示,随着年龄增长,利福平耐药风险逐渐降低,OR值从<25岁组的2.778下降至45~岁组的1.654(均P<0.001)。流动人口、居住在主城都市区、职业为工人及民工是复治肺结核患者利福平耐药的危险因素,差异均具有统计学意义(均P<0.05)。结论虽然重庆市复治肺结核患者利福平耐药检出率逐年下降,但形势依然严峻,需重点关注流动人口、低龄、居住在主城都市区和工人及民工相关人群。

利福平耐药结核病患者表型药敏试验结果分析及与Xpert MTB/RIF结果比较

目的分析利福平(RIF)耐药结核病患者表型药敏试验结果,并与结核分枝杆菌(MTB)及RIF耐药菌检测(Xpert MTB/RIF)结果进行对比。方法回顾性收集2019年1月至2021年12月昆明市第三人民医院收治的经Xpert MTB/RIF证实RIF耐药的288例结核病患者的临床资料,其中MTB培养阴性63例,MTB培养阳性225例。除8例患者因联系不上未行药敏试验外,其余213例MTB培养阳性患者均采用微孔板比例法进行药敏试验。比较表型药敏检测结果及其与Xpert MTB/RIF结果的差异。结果行药敏试验的213例RIF耐药结核病患者中,MDR患者比例最高,占53.5%(114/213),广泛耐药患者占22.5%(48/213);男性耐药患者比例[65.7%(140/213)]高于女性[34.3%(73/213)],但差异无统计学意义(P>0.05);RIF耐药结核病患者中,初治患者耐药发生率较高;在MDR和广泛耐药患者中,复治患者耐药发生率均高于初治患者,差异均有统计学意义(χ^(2)=5.648、13.385,P<0.05)。一线抗结核药物耐药率从高到低依次为RIF、利福喷汀、异烟肼、链霉素、乙胺丁醇,其耐药率分为96.7%(206/213)、96.7%(206/213)、76.1%(162/213)、26.8%(57/213)、20.2%(43/213)二线抗结核药物耐药率从高到低依次为利福布汀、莫西沙星、左氧氟沙星、对氨基水杨酸钠、阿米卡星、帕司烟肼、卡那霉素、卷曲霉素、丙硫异烟胺、克拉霉素、氯法齐明,耐药率分别为93.8%(200/213)、19.2%(41/213)、18.8%(40/213)、6.1%(13/213)、4.7%(10/213)、4.7%(10/213)、4.7%(10/213)、4.2%(9/213)、1.4%(3/213)、1.4%(3/213)、0.9%(2/213)。进行表型药敏试验的213例患者中,有7例(3.3%)显示基因耐药表型敏感,206例(96.7%)显示基因耐药表型耐药。结论氟喹诺酮类耐药率在二线药物中耐药率最高,故应加强Xpert MTB/RIF检测和抗结核药物表型药敏试验,以指导临床用药。

2019—2021年宜春地区患者结核分枝杆菌利福平耐药株基因型分析研究

目的:探究2019—2021年宜春地区结核分枝杆菌利福平耐药株基因型。方法:选择2019年1月—2021年12月于宜春市人民医院接受治疗的肺结核患者100例,采集所有患者痰液样本进行检测。分析结核分枝杆菌分离情况及耐药性,另分析利福平耐药株基因型。结果:100例患者中共分离出结核分枝杆菌47株,分离率为47.00%,2019、2020、2021年结核分枝杆菌分离率分别为33.33%、45.95%、54.76%。2019年分离出结核分枝杆菌7株,利福平、异烟肼、链霉素耐药发生率分别为42.86%、28.57%、28.57%;2020年分离出结核分枝杆菌17株,利福平、异烟肼、链霉素耐药发生率分别为58.82%、29.41%、11.76%;2021年分离出结核分枝杆菌23株,利福平、异烟肼、链霉素耐药发生率分别为60.87%、21.74%、17.39%。结核分枝杆菌对利福平耐药率最高。经rpoB基因测序可见27株利福平耐药株均发生rpoB基因变异,基因突变率为100%(27/27),突变基因位点主要位于509~533位。结论:2019—2021年宜春地区结核分枝杆菌感染率呈逐年上升趋势,结核分枝杆菌感染患者对利福平存在较高的耐药性,且rpoB基因位点突变的发生与利福平耐药间存在密切联系。

耐多药和利福平耐药肺结核治疗结局的Nomogram风险预测模型构建

目的:探讨耐多药和利福平耐药肺结核(MDR/RR-TB)住院患者的治疗结局及影响因素,构建并评价Nomogram风险预测模型。方法:收集2019年1月1日至2019年12月31日昆明市第三人民医院MDR/RR-TB住院患者临床资料并电话随访。采用χ^(2)检验和多因素Logistic回归分析筛选治疗结局的影响因素,构建Nomogram模型并验证。结果:141例患者中,治疗成功79例(占56.03%),不良转归62例(占43.97%)。多因素Logistic回归分析结果显示,糖尿病、血液系统疾病和农村居住是MDR/RR-TB患者治疗结局的危险因素,初中及以上文化程度是MDR/RR-TB患者治疗结局的保护因素。基于上述4个相关影响因素构建Nomogram模型,受试者操作特征曲线下面积为0.752(95%CI:0.673~0.832),敏感度为0.667,特异度为0.831。采用Bootstrap法重抽样1000次行内部验证,平均绝对误差为0.041,预测值和实际值一致性较好。Hosmer-Lemeshow检验结果表明,模型拟合度较好(χ^(2)=8.119,P=0.322)。决策曲线显示Nomogram模型在高风险阈值范围(0.14~0.81)时,临床实用价值较好。结论:构建的Nomogram模型具有较好的预测性、一致性及临床实用性,可为临床治疗MDR/RR-TB提供一定的科学参考。

探针熔解曲线在耐药结核病快速筛查中的临床应用研究

目的研究探针熔解曲线在耐药结核病快速筛查中的临床应用价值。方法选取2020年1月—2021年3月镇江市第三人民医院收治的378例肺结核患者为研究对象,依次完成传统罗氏固体药物敏感性检测(比例法)、探针熔解曲线技术检测常用的6种药物耐药结果,包含利福平、异烟肼、乙胺丁醇、链霉素、氧氟沙星、阿米卡星,和比例法进行对比,计算探针熔解曲线技术检测6种药物的敏感度、特异度、阳性预测值、阴性预测值、符合率与约登指数。结果与比例法作比较,熔解曲线技术检测利福平耐药性的敏感度、特异度、阳性预测值、阴性预测值、符合率、约登指数分别为91.70%、98.10%、61.10%、99.70%、97.90%、0.898;异烟肼是87.90%、94.20%、59.20%、98.80%、93.65%、0.821;乙胺丁醇是87.50%、97.03%、38.89%、99.72%、96.83%、0.845;链霉素是91.30%、98.19%、87.50%、98.79%、97.35%、0.895;氧氟沙星是94.74%、98.89%、81.82%、99.72%、98.68%、0.936;阿米卡星是80.00%、99.46%、66.67%、99.73%、99.21%、0.795。结论探针熔解曲线在耐药结核病快速筛查中应用,具有较高敏感度及特异度,有利于临床早期识别耐药现象。

富马酸贝达喹啉联合2HVZE/4HVE对利福平肺结核患者的影响

目的分析富马酸贝达喹啉联合2HVZE/4HVE对利福平肺结核患者痰菌转阴率及血清细胞因子水平的影响。方法选取86例利福平肺结核患者,按照随机数字表法分为A组和B组,每组43例。B组采用2HVZE/4HVE方案治疗,A组采用富马酸贝达喹啉联合2HVZE/4HVE治疗。比较两组临床疗效、空洞闭合率、病灶吸收率、痰菌转阴率、免疫功能指标、血清降钙素原(PCT)、白细胞介素-6(IL-6)、肿瘤坏死因子-α(TNF-α)、谷胱甘肽S-转移酶-π(GSTπ)水平、不良反应发生率。结果治疗6个月后,A组总有效率、空洞闭合率、病灶吸收率、痰菌转阴率、免疫功能指标水平均高于B组,血清GSTπ、IL-6、TNF-α、PCT水平均低于B组,差异有统计学意义(P<0.05)。两组不良反应总发生率比较,差异无统计学意义(P>0.05)。结论富马酸贝达喹啉辅助治疗利福平肺结核患者,效果显著,缓解临床症状,调节免疫功能,促进病情改善。