KAUROV, Iosif, Jiří HELLER, Sebastian DEISENHAMMER, David POTĚŠIL, Zbyněk ZDRÁHAL and Hassan HASHIMI. The essential cysteines in the CIPC motif of the thioredoxin-like Trypanosoma brucei MICOS subunit TbMic20 do not form an intramolecular disulfide bridge in vivo. MOLECULAR AND BIOCHEMICAL PARASITOLOGY. NETHERLANDS: ELSEVIER, 2022, vol. 248, MAR, p. "111463", 10 pp. ISSN 0166-6851. Available from: https://dx.doi.org/10.1016/j.molbiopara.2022.111463. |
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@article{1858757, author = {Kaurov, Iosif and Heller, Jiří and Deisenhammer, Sebastian and Potěšil, David and Zdráhal, Zbyněk and Hashimi, Hassan}, article_location = {NETHERLANDS}, article_number = {MAR}, doi = {http://dx.doi.org/10.1016/j.molbiopara.2022.111463}, keywords = {Trypanosoma Mitochondrion MICOS Protein import Intermembrane space Oxidative folding}, language = {eng}, issn = {0166-6851}, journal = {MOLECULAR AND BIOCHEMICAL PARASITOLOGY}, title = {The essential cysteines in the CIPC motif of the thioredoxin-like Trypanosoma brucei MICOS subunit TbMic20 do not form an intramolecular disulfide bridge in vivo}, url = {http://www.sciencedirect.com/science/article/pii/S0166685122000172}, volume = {248}, year = {2022} }
TY - JOUR ID - 1858757 AU - Kaurov, Iosif - Heller, Jiří - Deisenhammer, Sebastian - Potěšil, David - Zdráhal, Zbyněk - Hashimi, Hassan PY - 2022 TI - The essential cysteines in the CIPC motif of the thioredoxin-like Trypanosoma brucei MICOS subunit TbMic20 do not form an intramolecular disulfide bridge in vivo JF - MOLECULAR AND BIOCHEMICAL PARASITOLOGY VL - 248 IS - MAR SP - "111463" EP - "111463" PB - ELSEVIER SN - 01666851 KW - Trypanosoma Mitochondrion MICOS Protein import Intermembrane space Oxidative folding UR - http://www.sciencedirect.com/science/article/pii/S0166685122000172 N2 - The mitochondrial protein import machinery of trypanosomatids is highly divergent from that of the well-studied models such as baker's yeast. A notable example is that the central catalyst of the mitochondrial intermembrane space import and assembly pathway (MIA), named Mia40, is missing in trypanosomatids. Mia40 works in a two-step process. First it recognizes by direct binding reduced MIA substrate proteins and then catalyzes their oxidative folding to produce intramolecular disulfide bridges. It was recently proposed that a thioredoxin-like subunit of the trypanosomal mitochondrial contact site and cristae organizing system (MICOS) called TbMic20 may be the Mia40 replacement. Our study performed on procyclic stage of the parasite revealed that each of the two cysteines in TbMic20's active site is essential for the stability of MIA substrate proteins although they do not form a disulfide bridge in vivo. The two cysteines of Mia40 & PRIME;s active site form an intramolecular di-sulfide bridge at steady state, which is a prerequisite for its oxidative folding of MIA substrates. Thus, we conclude that TbMic20 is unlikely to represent a bona fide Mia40 replacement and plays a still unresolved role in the stability and/or import of MIA substrates in trypanosomatids. Despite this, the effect of TbMic20 depletion and mutation indicates that the trypanosomal MICOS complex still plays a vital role in the maturation and/or stability of proteins imported by the MIA pathway. ER -
KAUROV, Iosif, Jiří HELLER, Sebastian DEISENHAMMER, David POTĚŠIL, Zbyněk ZDRÁHAL and Hassan HASHIMI. The essential cysteines in the CIPC motif of the thioredoxin-like Trypanosoma brucei MICOS subunit TbMic20 do not form an intramolecular disulfide bridge in vivo. \textit{MOLECULAR AND BIOCHEMICAL PARASITOLOGY}. NETHERLANDS: ELSEVIER, 2022, vol.~248, MAR, p.~''111463'', 10 pp. ISSN~0166-6851. Available from: https://dx.doi.org/10.1016/j.molbiopara.2022.111463.
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