Morris Rowan P, Nguyen Liem, Gatfield John, Visconti Kevin, Nguyen Kien, Schnappinger Dirk, Ehrt Sabine, Liu Yang, Heifets Leonid, Pieters Jean, Schoolnik Gary, Thompson Charles J
Department of Medicine, Division of Infectious Diseases and Geographic Medicine, Stanford Medical School, Stanford, CA 94305, USA.
Proc Natl Acad Sci U S A. 2005 Aug 23;102(34):12200-5. doi: 10.1073/pnas.0505446102. Epub 2005 Aug 15.
Chemotherapeutic options to treat tuberculosis are severely restricted by the intrinsic resistance of Mycobacterium tuberculosis to the majority of clinically applied antibiotics. Such resistance is partially provided by the low permeability of their unique cell envelope. Here we describe a complementary system that coordinates resistance to drugs that have penetrated the envelope, allowing mycobacteria to tolerate diverse classes of antibiotics that inhibit cytoplasmic targets. This system depends on whiB7, a gene that pathogenic Mycobacterium shares with Streptomyces, a phylogenetically related genus known as the source of diverse antibiotics. In M. tuberculosis, whiB7 is induced by subinhibitory concentrations of antibiotics (erythromycin, tetracycline, and streptomycin) and whiB7 null mutants (Streptomyces and Mycobacterium) are hypersusceptible to antibiotics in vitro. M. tuberculosis is also antibiotic sensitive within a monocyte model system. In addition to antibiotics, whiB7 is induced by exposure to fatty acids that pathogenic Mycobacterium species may accumulate internally or encounter within eukaryotic hosts during infection. Gene expression profiling analyses demonstrate that whiB7 transcription determines drug resistance by activating expression of a regulon including genes involved in ribosomal protection and antibiotic efflux. Components of the whiB7 system may serve as attractive targets for the identification of inhibitors that render M. tuberculosis or multidrug-resistant derivatives more antibiotic-sensitive.
结核分枝杆菌对大多数临床应用抗生素的固有耐药性严重限制了治疗结核病的化疗选择。这种耐药性部分源于其独特细胞壁的低渗透性。在此,我们描述了一个互补系统,该系统可协调对已穿透细胞壁的药物的耐药性,使分枝杆菌能够耐受多种抑制细胞质靶点的抗生素。该系统依赖于whiB7基因,致病分枝杆菌与链霉菌属(一个在系统发育上相关且作为多种抗生素来源而闻名的属)共享该基因。在结核分枝杆菌中,whiB7由亚抑制浓度的抗生素(红霉素、四环素和链霉素)诱导,并且whiB7基因敲除突变体(链霉菌属和分枝杆菌属)在体外对抗生素高度敏感。在单核细胞模型系统中,结核分枝杆菌对抗生素也敏感。除了抗生素外,接触致病分枝杆菌在感染期间可能在其内部积累或在真核宿主中遇到的脂肪酸也可诱导whiB7。基因表达谱分析表明,whiB7转录通过激活一个调控子的表达来决定耐药性,该调控子包括参与核糖体保护和抗生素外排的基因。whiB7系统的组成部分可能是鉴定使结核分枝杆菌或耐多药衍生物对抗生素更敏感的抑制剂的有吸引力的靶点。