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The emergence of Beijing family genotypes of Mycobacterium tuberculosis and low-level protection by bacille Calmette–Guérin (BCG) vaccines: is there a link?

机译:北京结核分枝杆菌家族基因型的出现和卡介苗的低水平保护:BCG疫苗有联系吗?

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摘要

The world is confronted with major tuberculosis (TB) outbreaks at a time when the protection of bacillus Calmette–Guérin (BCG) vaccine has become inconsistent and controversial. Major TB outbreaks are caused by a group of genetically similar strains of Mycobacterium tuberculosis (Mtb) strains, including the Beijing family genotypes. The Beijing family genotypes exhibit important pathogenic features such high virulence, multi-drug resistance and exogenous reinfection. These family strains have developed mechanisms that modulate/suppress immune responses by the host, such as inhibition of apoptosis of infected macrophages, diminished production of interleukin (IL)-2, interferon (IFN)-γ, tumour necrosis factor (TNF)-α and elevated levels of IL-10 and IL-18. They demonstrate distinct expression of proteins, such as several species of α-crystallin (a known Mtb virulence factor), but decreased expression of some antigens such as heat shock protein of 65 kDa, phosphate transport subunit S and a 47-kDa protein. In addition, the Beijing family strains specifically produce a highly bioactive lipid (a polyketide synthase)-derived phenolic glycolipid. This altered expression of proteins/glycolipids may be important factors underlying the success of the Beijing family strains. The Beijing family strains are speculated to have originated from South-east Asia, where BCG vaccination has been used for more than 60 years. The hypothesis that mass BCG vaccination may have been a selective factor that favoured genotypic and phenotypic characteristic acquired by the Beijing family strains is discussed.
机译:当卡介苗(BCG)疫苗的保护方法变得前后矛盾并引起争议时,世界就面临着重大结核病(TB)的爆发。主要的结核病暴发是由一组结核分枝杆菌(Mtb)遗传相似的菌株引起的,包括北京家族的基因型。北京家族的基因型表现出重要的致病特征,如高毒力,多药耐药性和外源性再感染。这些家族菌株已开发出调节/抑制宿主免疫应答的机制,例如抑制感染巨噬细胞的凋亡,降低白介素(IL)-2,干扰素(IFN)-γ,肿瘤坏死因子(TNF)-α的产生。 IL-10和IL-18水平升高。他们证明了蛋白质的独特表达,例如几种α-晶状蛋白(一种已知的Mtb毒力因子),但是某些抗原的表达却降低了,例如65 kDa的热激蛋白,磷酸转运亚基S和47 kDa的蛋白。此外,北京家族菌株特异性产生高生物活性脂质(聚酮化合物合酶)衍生的酚糖脂。蛋白质/糖脂表达的这种改变可能是北京家族菌株成功的重要因素。据推测,北京家族菌株起源于东南亚,该地区使用卡介苗接种已有60多年的历史了。讨论了BCG大规模疫苗接种可能是有利于北京家庭菌株获得的基因型和表型特征的选择因素的假说。

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