Malmsheimer Silke, Daher Wassim, Tasrini Yara, Hamela Claire, Aguilera-Correa John Jairo, Chalut Christian, Hatfull Graham F, Kremer Laurent
Centre National de la Recherche Scientifique UMR 9004, Institut de Recherche en Infectiologie de Montpellier (IRIM), Université de Montpellier, Montpellier, France.
INSERM, IRIM, Montpellier, France.
mBio. 2024 Dec 11;15(12):e0297024. doi: 10.1128/mbio.02970-24. Epub 2024 Oct 30.
Mycobacteria produce a large repertoire of surface-exposed lipids with major biological functions. Among these lipids, trehalose polyphleates (TPPs) are instrumental in the infection of by the therapeutic phage BPs. However, while the biosynthesis and transport of TPPs across the membrane by MmpL10 have been reported, the role of TPPs in host infection remains enigmatic. Here, we addressed whether the loss of TPPs influences interactions with macrophages and the virulence of . As anticipated, the deletion of in smooth (S) and rough (R) variants of abrogated TPP production, which was rescued upon gene complementation. Importantly, infection of human THP-1 cells with the mutants was associated with decreased intramacrophage survival and a reduced proportion of infected cells. The rough mutant showed an impaired capacity to block phagosomal acidification and was unable to co-localize with Galectin-3, a marker of phagosomal membrane damage. This suggests that TPPs participate, directly or indirectly, in phagolysosomal fusion and in phagosomal membrane damage to establish cytosolic communication. The TPP defect that affects the fitness and virulence of was further demonstrated in zebrafish embryos using a rough clinical strain resistant to phage BPs and harboring a frameshift mutation in . Infection with this strain was correlated with a slight decrease in embryo survival and a reduced bacterial burden as compared to the corresponding parental and complemented derivatives. Together, these results indicate that TPPs are important surface lipids contributing to the pathogenicity of .IMPORTANCETrehalose polyphleates (TPPs) are complex lipids associated with the mycobacterial cell surface and were identified 50 years ago. While the TPP biosynthetic pathway has been described recently, the role of these lipids in the biology of mycobacteria remains yet to be established. The wide distribution of TPPs across mycobacterial species suggests that they may exhibit important functions in these actinobacteria. Here, we demonstrate that an emerging multidrug-resistant pathogen that causes severe lung diseases in cystic fibrosis patients, requires TPPs for survival in macrophages and virulence in a zebrafish model of infection. These findings support the importance of this underexplored family of lipids in mycobacterial pathogenesis.
分枝杆菌产生大量具有主要生物学功能的表面暴露脂质。在这些脂质中,海藻糖多聚分枝酸酯(TPPs)在治疗性噬菌体BPs感染过程中发挥作用。然而,虽然已经报道了MmpL10介导TPPs的生物合成及其跨膜转运,但TPPs在宿主感染中的作用仍然不明。在此,我们研究了TPPs的缺失是否会影响与巨噬细胞的相互作用以及分枝杆菌的毒力。正如预期的那样,在光滑(S)和粗糙(R)变种的分枝杆菌中缺失该基因会消除TPP的产生,而基因互补后则可恢复。重要的是,用该突变体感染人THP-1细胞与巨噬细胞内存活率降低以及被感染细胞比例减少有关。粗糙突变体显示出阻断吞噬体酸化的能力受损,并且无法与作为吞噬体膜损伤标志物的半乳糖凝集素-3共定位。这表明TPPs直接或间接参与吞噬溶酶体融合以及吞噬体膜损伤以建立胞质通讯。使用对噬菌体BPs耐药且在该基因中存在移码突变的粗糙临床菌株,在斑马鱼胚胎中进一步证明了影响分枝杆菌适应性和毒力的TPP缺陷。与相应的亲本及互补衍生物相比,感染该菌株与胚胎存活率略有下降和细菌载量减少相关。总之,这些结果表明TPPs是有助于分枝杆菌致病性的重要表面脂质。
重要性
海藻糖多聚分枝酸酯(TPPs)是与分枝杆菌细胞表面相关的复杂脂质,于50年前被鉴定。虽然最近已经描述了TPP的生物合成途径,但这些脂质在分枝杆菌生物学中的作用仍有待确定。TPPs在分枝杆菌物种中的广泛分布表明它们可能在这些放线菌中发挥重要功能。在此,我们证明了一种在囊性纤维化患者中引起严重肺部疾病的新兴多重耐药病原体,在巨噬细胞中存活以及在斑马鱼感染模型中的毒力需要TPPs。这些发现支持了这个未被充分探索的脂质家族在分枝杆菌发病机制中的重要性。
