The accumulation of methylated porphyrins in dormant cells of Mycolicibacterium smegmatis is accompanied by a decrease in membrane fluidity and an impede of the functioning of the respiratory chain

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-01-09 DOI:10.1016/j.bbamem.2024.184270
Ivan A. Gligonov , Daria I. Bagaeva, Galina R. Demina, Galina N. Vostroknutova, Dmitriy S. Vorozhtsov, Arseny S. Kaprelyants, Alexander P. Savitsky, Margarita O. Shleeva
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Abstract

Transition of Mycolicibacterium smegmatis (Msm) and Mycobacterium tuberculosis to dormancy in vitro is accompanied by an accumulation of free methylated forms of porphyrins (tetramethyl coproporphyrin – TMC) localized in the cell wall of dormant bacteria. A study of the fluorescence anisotropy of BODIPY based fluorescent probes on individual cell level using confocal microscope revealed significant changes in this parameter for BODIPY FL C16 from 0.05 to 0.22 for vegetative and dormant Msm cells correspondingly. Similarly, the increase of TMC concentration in vegetative Msm cells grown in the presence of 5-aminolevulinic acid (a known inducer of porphyrin synthesis) resulted in an increase of BODIPY FL C16 anisotropy. These changes in TMC concentration and membrane fluidity were accompanied by an inhibition of the activity of the respiratory chain measured by oxygen consumption and a reduction of the DCPIP redox acceptor. During the first 8 h of the reactivation of the dormant Msm cells, the porphyrin content and probe fluorescent anisotropy returned to the level for vegetative bacteria. We suggested that upon transition to dormancy, an accumulation of TMC in membranes leads to a decrease in membrane fluidity, resulting in an inhibition of the respiratory chain activity. However, direct interactions of TMC with membrane bound enzymes cannot also be excluded. This, in turn, may result in the down regulation of many metabolic energy-dependent reactions as a part of mechanisms accompanying the transition to a hypometabolic state of mycobacteria.

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烟曲霉菌休眠细胞中甲基化卟啉的积累伴随着膜流动性的降低和呼吸链功能的阻碍
伴随着休眠细菌细胞壁中游离甲基化形式的卟啉(四甲基共卟啉 - TMC)的积累,烟曲霉分枝杆菌(Msm)和结核分枝杆菌在体外进入休眠状态。使用共聚焦显微镜对基于 BODIPY 的荧光探针在单个细胞水平上的荧光各向异性进行研究后发现,BODIPY FL C16 在无性繁殖细胞和休眠 Msm 细胞中的荧光各向异性参数从 0.05 到 0.22 有了显著变化。同样,在 5-氨基乙酰丙酸(一种已知的卟啉合成诱导剂)存在下生长的无性 Msm 细胞中 TMC 浓度的增加也导致 BODIPY FL C16 各向异性的增加。在 TMC 浓度和膜流动性发生变化的同时,以耗氧量和 DCPIP 氧化还原受体的减少来衡量的呼吸链活性也受到了抑制。在休眠 Msm 细胞重新激活的前 8 小时,卟啉含量和探针荧光各向异性恢复到无性繁殖细菌的水平。我们认为,过渡到休眠状态后,膜中 TMC 的积累会导致膜流动性降低,从而抑制呼吸链的活性。不过,也不能排除 TMC 与膜结合酶直接相互作用的可能性。这反过来又可能导致许多依赖新陈代谢能量的反应受到抑制,成为分枝杆菌过渡到低代谢状态的机制的一部分。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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