利福霉素衍生物Rifabutin的临床药理研究进展

Rifabutin(RBT)是一种类似于利福平(RIF)的利福霉素衍生物。1992年被美国FDA批准用于治疗和预防发生在AIDS患者上的鸟分枝杆菌(MAC)感染,随后许多国家相继批准使用该药。但是后来RBT已不仅被用于预防治疗MAC,还用于治疗肺结核以及幽门螺杆菌(HP)感染。正是由于该药相对于其他利福霉素类药物的高度亲脂性和较弱的CYP450诱导作用使得它成功应用于临床多种疾病的治疗,尤其是和多种抗生素联合用药时,不仅部分解决了传统抗生素的细菌耐受性问题而且增加了临床联合用药的安全性。本文旨在阐述有关的Ri-fabutin的临床药理以及相关方面的研究进展,以便指导今后临床用药。

Correlation between rpoB gene mutation in Mycobacterium avium subspecies paratuberculosis and clinical rifabutin and rifampicin resistance for treatment of Crohn’s disease

AIM： To investigate overlapping regions of the rpoB gene previously involved with rifamycin resistance in M. tuberculosis and seek correlation between rpoB mutations in dinical MAP strains with susceptibility to RIF and RFB. METHODS： We designed a molecular-based PCR method for the evaluation of rifabutin （RFB） and rifampicin （RIF） resistance based on probable determinant regions within the rpoB gene of MAP, including the 81 bp variable site located between nucleotides 1363 and 1443. The minimum inhibitory concentration （MIC） for RIF was also determined against 11 MAP isolates in attempt to seek correlation with rpoB sequences. RESULTS： We determined that MAP strain 18 had an MIC of 〉 30 mg/L and ≤ 5 mg/L for RIF and RFB respectively, and a significant and novel rpoB mutation C1367T, compared to an MIC of ≤ 1.0 mg/L for both drugs in the wild type MAP. The 30-fold increase in the MIC was a direct result of the rpoB mutation C1367T, which caused an amino acid change Thr456 to Ile456 in the drug＇s binding site. In addition, MAP strain 185 contained five silent rpoB mutations and exhibited an MIC comparable to the wild-type. Moreover, our in vitro selected mutation in MAP strain UCF5 resulted in the generation of a new resistant strain （UCF5-RIF16r） that possessed T1442C rpoB mutation and an MIC 〉 30 mg/L and 〉 10 mg/L for RIF and RFB respectively. Sequencing of the entire rpoB gene in MAP strains UCF4, 18, and UCF5-RIF16r revealed an rpoB mutation A2284C further downstream of the 81 bp variable region in UCF4, accounting for observed slight increase in MIC. In addition, no other significant mutations were found in strains 18 and UCF-RIF16r. CONCLUSION： The data clearly illustrates that clinical and in vitro-selected MAP mutants with rpoB mutations result in resistance to RIF and RFB, and that a single amino acid change in the beta subunit may have a significant impact on RIF resistance. Unconventional drug susceptibility testing such as our molecular approach will be beneficial for evaluation of antibiotic effectiveness. This molecular approach may also serve as a model for other drugs used for treatment of MAP infections.

Rifabutin as salvage therapy for Helicobacter pylori eradication:Cornerstones and novelties

When several Helicobacter pylori eradication treatments fail,guidelines recommend a cultured guided approach;however,culture is not widely available.Therefore,a rifabutin based regimen could be the best solution.Rifabutin indeed shows a low rate of antibiotic resistance.Rifabutin is generally used in combination with amoxicillin in a triple therapy,with eradication rates about 80%in third-line regimens.The ideal duration of this therapy should range between 10 and 12 d.Combinations with antibiotics other than amoxicillin have demonstrated even better results,such as vonoprazan,which is a type of novel acid suppressor drug.Finally,a new formulation of triple therapy in a single capsule is under investigation,which is a field that deserves further investigation.Some notes of caution about rifabutin should be mentioned.This drug is used to treat tuberculosis or atypical mycobacteria;therefore,before starting a rifabutin-based eradication regimen,Mycobacterium tuberculosis infection should be thoroughly tested,since its use could promote the development of antibiotic resistance,thus affecting its effectiveness against Koch’s bacillus.Additionally,some serious side effects must be evaluated before starting any rifabutin-based therapy.Adverse effects include fever,nausea,vomiting and bone marrow suppression.For this reason,full blood count surveillance is required.

利福布汀在获得性免疫缺陷综合征患者中引起的前房积脓型葡萄膜炎

目的 提高对利福布汀相关性前房积脓型葡萄膜炎的认识、诊断及治疗能力。方法 回顾性系列病例研究。回顾分析14例(24眼)获得性免疫缺陷综合征(AIDS)合并结核分枝杆菌复合群(MTC)或非结核分枝杆菌(NTM)感染患者应用利福布汀后发生前房积脓型葡萄膜炎的眼部临床表现及其治疗随访结果。结果本组病例中,男性13例、女性1例;年龄24~78岁,平均(42.50±14.29)岁;体重44~73 kg,平均(54.21±9.07)kg。CD_(4)^(+)T淋巴细胞(19~260)个/μL,平均(91.07±59.36)个/μL。临床表现:单眼或双眼(同时或先后)急性发作眼红、眼痛、畏光、视力明显下降。大量角膜后沉积物,前房纤维素性渗出,前房积脓,虹膜后粘连。眼底无法窥及。B超示玻璃体大量团状强回声影。治疗:14例均给予局部糖皮质激素类药物、扩瞳剂治疗。1例除局部治疗外给予全身应用甲泼尼龙40 mg, 3 d。14例(24眼)患者眼部病变均迅速完全缓解,8眼葡萄膜炎复发。结论 随着利福布汀的广泛应用,利福布汀相关性葡萄膜炎日益增多,医师应重视这种潜在的并发症。认识此病,可以避免前房穿刺、玻璃体注药、玻璃体切除术等有创操作。及时治疗可大大提高患者视力,减少并发症的发生。

利福布汀影响伏立康唑血药浓度1例并文献复习

目的了解联合应用利福布汀对伏立康唑血药浓度的影响。方法对我院1例利福布汀、异烟肼等抗结核药与伏立康唑联合应用,伏立康唑的血药浓度进行分析,并以“伏立康唑”、“利福布汀”为主题词检索万方、维普和中国知网数据库,以“Voriconazole”、“Rifabutin”为主题词检索Pubmed数据库,检索国内外报道的利福布汀影响伏立康唑血药浓度的病例,筛选并总结分析病例资料。结果本院报道的病例中,患者联合使用利福布汀0.3 g,1日1次和伏立康唑200 mg,1日2次,4个月,结果伏立康唑的血药浓度为0.00μg·mL^(-1)。文献检索到2例案例报道,利福布汀可诱导伏立康唑的体内代谢,但在治疗浓度监测下进行治疗方案调整,可达到有效浓度。结论利福布汀对细胞色素P-450酶(CYP450)的诱导作用低于利福平,与伏立康唑合用时,需要在治疗药物监测下,调整伏立康唑给药方案;同时伏立康唑通过抑制CYP3A4,可增加利福布汀稳态峰浓度(C_(max))和药-时曲线下面积(AUC),需要密切监测患者的全血细胞计数和与利福布汀有关的不良反应。

利福布汀治疗耐多药肺结核临床观察

目的评价利福布汀治疗耐多药肺结核的临床有效性和安全性。方法采用为期18个月的随机、开放、对照临床试验。试验组:3BPaVEThAk/6BPaVETh/9BPaVE;对照组:3L2PaVEThAk/6L2PaVETh/9L2PaVE。结果试验组在各阶段的病灶显吸率与空洞闭合率均高于平行对照组,且临床症状与体征的改善也优于对照组。其中试验组在3个月时病灶有效率达100.0%(9/9),在6个月时痰结核菌阴转率达100.0%,与对照组同期经χ2检验比较,差异有显著性(P<0.05)。利福布汀不良反应为抗结核药物中常见的副反应。结论利福布汀治疗耐多药肺结核的疗效优于利福喷丁,且具有较好的安全性,对治疗耐多药肺结核具有很大的潜力。

利福布汀联合抗病毒药物治疗艾滋病合并结核病的临床研究

目的:探究利福布汀联合抗病毒药物在治疗艾滋病合并结核病的临床效果。方法:将本院感染科在2014年1月至2015年12月期间收治的艾滋病合并肺结核患者80例作为本次研究对象,根据临床用药的不同分为观察组和对照组,两组患者各40例,观察组实施含福布汀的抗痨方案+含依菲韦伦或克力芝抗病毒方案,对照组实施含利福平的抗痨方案+含依菲韦伦抗病毒方案,两组患者均进行抗结核治疗和抗艾滋病毒治疗,观察两组患者抗结核疗效、抗病毒疗效以及总不良反应情况。结果:研究组在抗结核治疗有效率、痰检转阴率、肺部空洞闭合率及肺部病灶吸收明显高于对照组(P<0.05);两组患者治疗前的CD4+T淋巴细胞差异无统计学意义(P>0.05),在经过治疗后,两组患者的CD4+T淋巴细胞均有明显上升,且研究组明显高于对照组(P<0.05);研究组患者发生免疫重建炎症综合征情况以及总不良反应情况明显低于对照组(P<0.05)。结论:利福布汀联合抗病毒治疗肺结核合并的临床效果显著,可以有效提高患者的痊愈率,降低不良反应发生,减少免疫重建炎症综合征的发生,增加抗结核及抗病毒疗效。

利福平和利福布汀对结核分枝杆菌交叉耐药率的初步探讨

目的通过对结核分枝杆菌MIC的测定,初步探讨利福平和利福布汀两药间的交叉耐药率。方法利用Alarmar Blue法(Alamar blue susceptibility test,MABA)检测116株结核分枝杆菌临床分离株对利福平和利福布汀的体外MIC。结果 36株利福平敏感株均对利福布汀敏感;80株利福平耐药株中有58株对利福布汀也同时耐药(对利福布汀的MIC>0.5 ug/ml),利福平与利福布汀间的交叉耐药率为72.5%(58/80);同时对利福平和利福布汀耐药的菌株对两种药物的耐药程度呈现正相关。结论利福布汀较利福平有更好的体外抗菌活性。对于利福平耐药而利福布汀敏感的患者仍可选择利福布汀作为联合化疗的有效药物之一。

利福布汀联合莫西沙星治疗耐多药肺结核的近期疗效观察

目的:评价利福布汀和莫西沙星联合化疗方案对耐多药肺结核(MDR-PTB)的疗效。方法:将41例MDR-PTB患者随机分为两组,治疗组21例,采用以莫西沙星(M)、利福布汀(B)为主,联合力克肺疾(D)、丙硫异烟胺(Th)、阿米卡星(A)、乙胺丁醇(E)治疗;对照组20例,采用以左氧氟沙星(V)、利福喷汀(L)为主,联合D、Th、A、E治疗;疗程均为18个月。结果:治疗组痰菌阴转率为85.7%(18/21),对照组痰菌阴转率为55.0%(11/20),治疗组明显高于对照组(P<0.05)。治疗组和对照组病灶显吸率分别为47.6%(10/21)、25.0%(5/20),差异无统计学意义(P>0.05)。治疗组和对照组病灶有效率分别为81.0%(17/21)、50.0%(10/20),差异有统计学意义(P<0.05)。治疗组和对照组空洞闭合率分别为38.5%(5/13)、27.3%(3/11),差异无统计学意义(P>0.05),且两组间副作用比较差异无统计学意义(P>0.05)。结论:利福布汀联合莫西沙星方案治疗耐多药肺结核,具有促进痰菌阴转、病灶吸收和空洞闭合的作用,其安全性和耐受性良好。

利福布汀与人血清白蛋白相互作用的光谱研究

用荧光光谱法和圆二色谱法研究了利福布汀(RB)与人血清白蛋白(HSA)的相互作用.结果表明,RB与HSA之间的相互作用主要是疏水作用,作用机制是静态猝灭与动态猝灭的结合.其结合常数(Ka)在106数量级,说明RB和HSA有很强的结合.此外,探讨了金属离子(Cu2+,Zn2+,Mg2+和Ca2+)对RB与HSA结合常数的影响.同步荧光光谱和圆二色谱数据表明,RB可导致HSA的构象改变.

利福布丁较利福喷丁治疗耐多药肺结核的系统评价

目的评价利福布丁较利福喷丁治疗耐多药肺结核的有效性和安全性。方法计算机检索Medline、the Cochrane Cen-tral Register of Controlled Trials(CENTRAL)、CBM、CNKI、万方学位论文和会议数据库,Clinical trial.gov。检索日期截止至2008年10月。纳入利福布丁较利福喷丁治疗耐多药肺结核的随机对照试验。结果共纳入1个随机对照试验,完成治疗分析的和意向性治疗分析均表明在不同治疗阶段,利福布丁和利福喷汀两组病人痰菌阴转率、病灶显效率、病灶有效率比较,差异均无统计意义(p>0.05)。利福布丁和利福喷汀两组病人满疗程时空洞闭合率、不良事件发生率、肝损害发生率及严重不良事件发生率比较,差异也无统计学意义(p>0.05)。结论一个试验提示,利福布丁与利福喷丁治疗耐多药肺结核的疗效可能相似。需进一步开展随机、双盲、对照试验来确认两药对耐多药肺结核的相对效果。

利福喷丁与利福布汀对氯氮平血药浓度和疗效的影响

目的比较利福喷丁与利福布汀对氯氮平血药浓度和疗效的影响。方法采用随机数字表法将40例合并肺结核的精神分裂症患者分成利福喷丁组和利福布汀组，每组20例，两组患者在持续原来氯氮平剂量治疗〉2周的基础上分别联合应用利福喷丁（0．60g／次，2次／周）或利福布汀（O．15g／次，1次／d），共治疗6周。分别于联合用药前与联合用药后第2、6周末采用高效液相色谱法（HPIc）测定氯氮平血药浓度，同期以阳性和阴性症状量表（PANSS）评定精神症状。组内差异比较采用单因素方差分析，组间差异比较采用t检验，P〈0．05为差异有统计学意义。本研究是科研性的，旨在探索合并肺结核的精神分裂症患者的个体化治疗方案，实施前通过了伦理学委员会审查。结果利福布汀组患者联合用药前、联合用药后第2、6周末的氯氮平血药浓度分别为（247．5±106．8）、（279．0±165．3）和（239．4±157．1）ng／ml；PANSS总分分别为（70．95±14．98）、（71．30±15．47）和（73．75±15．29）分；阳性症状分分别为（13．95±5．81）、（14．15±6．07）和（15．75±5．51）分；阴性症状分分别为（22．15±7．80）、（22．00±7．01）和（21．5±6．95）分；一般精神病理分分别为（30．2±6．18）、（30．45±6．70）和（32．10±7．45）分，组内差异均无统计学意义（F值分别为0．42、0．20、0．58、0．14和0．46，P值均〉0．05）。利福喷丁组患者联合用药前和联合用药后第2、6周末的氯氮平血药浓度分别为（255．2±113．8）、（119．6±66．8）和（116．3±80．5）ng／ml，组内差异有显著统计学意义（F=15．8，P=0．000）。同期，其PANSS总分分别为（69．45±16．96）、（76．55±17．43）和（86．65±20．99）分；阳性症状分分别为（14．85±6．82）、（17．20±7．23）和（20．60±6．19）分；一般精神病理分分别为（29．75±7．07）、（32．95±6．35）和（36．40±8．46）分，组内差异均有统计学意义（F值分别为4．34、3．66和4．10，P值均〈0．05）。利福布汀组患者联合用药后第2、6周末的氯氮平血药浓度均明显高于同期利福喷丁组患者，组间差异均有显著统计学意义（f值分别为3．99和3．12，P值均〈0．01）；利福布汀组患者联合用药后第6周末的PANSS总分和阳性症状分均明显低于利福喷丁组，组间差异均有统计学意义（t值分别为-2．22和-2．62，P值均〈O．05）。结论与利福喷丁相比，利福布汀对氯氮平血药浓度及其抗精神病疗效的影响极小，利福布汀更适用于精神障碍伴肺结核患者的抗结核治疗。

广东地区结核分枝杆菌利福布丁耐药株rpoB全基因序列突变特征

目的分析广东地区结核分枝杆菌利福布丁耐药株rpoB全基因序列突变特征。方法常规比例法检出100株结核分枝杆菌利福布丁(rifabutin,RBU)耐药株,30株敏感株,扩增rpoB全基因序列并进行序列测定,Clustal×软件比对所测序列突变情况。结果利福布丁敏感株rpoB基因无突变;利福布丁耐药株有24种突变类型,121个突变位点,其中106个在利福平耐药决定区(rifampin resistance determining region,RRDR)之内,15个在RRDR之外,包括3个是单点突变(V176F,P206R,H323Y)和12个联合突变;常见突变位点分别是531(70%)和526(20%);两位点联合突变率21%,单点突变率79%。结论广东结核分枝杆菌敏感株rpoB基因不发生突变,利福布丁耐药株rpoB基因突变率100%,最常见突变位点分别是531和526。516、526和531之间不发生联合突变。RRDR之内鉴定出9种突变位点,RRDR之外鉴定出15个新突变位点,包括3个单点突变V176F,P206R和H323Y,位于rpoB基因起始端。

Third-line rescue therapy for Helicobacter pylori infection

H pylori gastric infection is one of the most prevalent infectious diseases worldwide. The discovery that most upper gastrointestinal diseases are related to Hpylori infection and therefore can be treated with antibiotics is an important medical advance. Currently, a first-line triple therapy based on proton pump inhibitor （PPI） or ranitidine bismuth citrate （RBC） plus two antibiotics （darithromycin and amoxicillin or nitroimidazole） is recommended by all consensus conferences and guidelines. Even with the correct use of this drug combination, infection can not be eradicated in up to 23% of patients. Therefore, several second line therapies have been recommended. A 7 d quadruple therapy based on PPI, bismuth, tetracycline and metronidazole is the more frequently accepted. However, with second-line therapy, bacterial eradication may fail in up to 40% of cases. When Hpylori eradication is striclly indicated the choice of further treatment is controversial. Currently, a standard third-line therapy is lacking and various protocols have been proposed. Even after two consecutive failures, the most recent literature data have demonsbated that Hpylori eradication can be achieved in almost all patients, even when antibiotic susceptibility is not tested. Different possibilities of empirical treatment exist and the available third-line strategies are herein reviewed.

利福霉素耐药结核分枝杆菌rpoB突变与利福布丁耐药水平的关系

目的研究利福霉素耐药结核分枝杆菌rpoB基因突变与利福布丁耐药水平的相关性。方法倍比稀释法测定64株利福霉素耐药及6株敏感菌株对利福布丁的最低抑菌浓度(MIC),并分析其对异烟肼的耐药情况。同时对rpoB全基因扩增后测序,分析rpoB突变位点和突变性质与利福布丁MICs高低及多重耐药的关系。结果 6株敏感株rpoB未突变,MICs为0.25～0.50 mg/L。64株耐药株rpoB突变率为100%。37株利福布丁高度耐药(MICs≥4 mg/L)株中,S531L突变27株,H526R突变和Y389C突变各2株,S531W、H526Y、Q513K、V176F、D516Y联合Q253R突变与D516G联合L511P突变各1株。17株中度耐药(MICs 2～4 mg/L)株中,S531L突变16株,D516G联合L511P和S509R突变1株。10株低度耐药(MICs 0.25～1 ng/L)株中,L533P、H526L、H526S、D516V、D516Y单点突变各2株。93.75%(60/64)的利福霉素耐药株对异烟肼耐药。结论检测rpoB突变即可初步筛选多重耐药结核分枝杆菌;中、高水平利福布丁耐药株以S531L突变占绝对优势,rpoB突变位点及突变类型与利福布丁耐药水平有一定相关性。

“Rescue” regimens after Helicobacter pylori treatment failure

Helicobacter pylori (H pylori) infection is the main cause of gastritis, gastroduodenal ulcer disease, and gastric cancer. After more than 20 years of experience in H pylori treatment, in my opinion, the ideal regimen to treat this infection is still to be found. Currently, apart from having to know first-line eradication regimens well, we must also be prepared to face treatment failures. Therefore, in designing a treatment strategy we should not focus on the results of primary therapy alone, but also on the final (overall) eradication rate. The choice of a "rescue" treatment depends on which treatment is used initially. If a clarithromycin- based regimen was used initially, a subsequent metronidazole-based treatment (quadruple therapy) may be used afterwards, and then a levofloxacin- based combination would be a third "rescue" option. Alternatively, it has recently been suggested that levofloxacin-based rescue therapy constitutes an encouraging second-line strategy, representing an alternative to quadruple therapy in patients with previous PPI-clarithromycin-amoxicillin failure, with the advantage of efficacy, simplicity and safety. In this case, a quadruple regimen may be reserved as a third-line rescue option. Finally, rifabutin-based rescue therapy constitutes an encouraging empirical fourth- line strategy after multiple previous eradication failures with key antibiotics such as amoxicillin, clarithromycin, metronidazole, tetracycline, and levofloxacin. Even after two consecutive failures, several studies have demonstrated that H pylori eradication can finally be achieved in almost all patients if several rescue therapies are consecutively given. Therefore, the attitude in H pylori eradication therapy failure, evenafter two or more unsuccessful attempts, should be to fight and not to surrender.

利福布汀胶囊溶出度测定

建立了紫外分光光度法测定利福布汀胶囊的溶出度。采用中国药典2000版附录ⅩC第一法,以0.01mol/L盐酸为溶出介质,转速100r/min,测定波长280nm。利福布汀在2.5～25mg/ml浓度范围内线性关系良好(r=0.9999),平均回收率98.3%(RSD 0.60%)。并以进口样品为对照进行溶出试验,结果表明两者前15min的溶出特性存在差异。

抗结核药物HPLC快速确证方法的研究

目的建立抗结核药物中异烟肼、吡嗪酰胺、对氨基水杨酸钠、乙硫异烟胺、丙硫异烟胺、利福平、利福喷丁、利福布丁等化合物的HPLC快速确证方法。方法采用AlltimaTMHP C18Rocket TM色谱柱;将以上化合物按物理性质分为3组,分别确定每组化合物的色谱分离体系;采用相对容量因子和紫外光谱相似度双指标进行定性;相对容量因子法进行定量分析。结果根据化合物的物理性质或结构,将其分组,确定每组化合物的色谱分离体系,以实现尽可能用较少的色谱体系分离较多化合物,减少HPLC分析过程中流动相的切换,加快药物分析速度;采用双指标进行定性,增加了HPLC定性的准确性;相对校正因子含量测定法,能有效减少对照品的使用,加快HPLC分析速度。结论抗结核药物HPLC快速确证方法快速、简便,适用于药品的快速检测,为HPLC法快速检测药品提供了指导原则。