Litcius/Paper detail

Functional cooperativity between the trigger factor chaperone and the ClpXP proteolytic complex

Kamran Rizzolo, Angela Yeou Hsiung Yu, Adedeji Ologbenla, Sa Rang Kim, Haojie Zhu, Koichiro Ishimori, Guillaume Thibault, Elisa Leung, Zhang Na, Mona Teng, Marta Haniszewski, Noha Miah, Sadhna Phanse, Zoran Minić, Sukyeong Lee, Julio Diaz Caballero, Mohan Babu, Francis Tsai, Tomohide Saio, Walid A. Houry

2021Nature Communications24 citationsDOIOpen Access PDF

Abstract

A functional association is uncovered between the ribosome-associated trigger factor (TF) chaperone and the ClpXP degradation complex. Bioinformatic analyses demonstrate conservation of the close proximity of tig, the gene coding for TF, and genes coding for ClpXP, suggesting a functional interaction. The effect of TF on ClpXP-dependent degradation varies based on the nature of substrate. While degradation of some substrates are slowed down or are unaffected by TF, surprisingly, TF increases the degradation rate of a third class of substrates. These include λ phage replication protein λO, master regulator of stationary phase RpoS, and SsrA-tagged proteins. Globally, TF acts to enhance the degradation of about 2% of newly synthesized proteins. TF is found to interact through multiple sites with ClpX in a highly dynamic fashion to promote protein degradation. This chaperone-protease cooperation constitutes a unique and likely ancestral aspect of cellular protein homeostasis in which TF acts as an adaptor for ClpXP.

Topics & Concepts

Chaperone (clinical)BiologyCell biologyProteolysisProtein degradationCooperativityrpoSProteaseGeneBiochemistryGene expressionEnzymeMedicinePathologyPromoterHeat shock proteins researchRNA and protein synthesis mechanismsToxin Mechanisms and Immunotoxins