Functional and structural diversification of incomplete phosphotransferase system in cellulose-degrading clostridia

Author:

Xu Tao123,Tao Xuanyu3ORCID,He Hongxi45,Kempher Megan L3,Zhang Siping6,Liu Xiaochun45,Wang Jun45,Wang Dongyu7,Ning Daliang3ORCID,Pan Chongle78,Ge Honghua45ORCID,Zhang Nannan45ORCID,He Yong-Xing6ORCID,Zhou Jizhong3910ORCID

Affiliation:

1. Section on Pathophysiology and Molecular Pharmacology, Joslin Diabetes Center , Boston, MA, USA

2. Department of Microbiology and Immunobiology, Harvard Medical School , Boston, MA, USA

3. Institute for Environmental Genomics, and Department of Microbiology and Plant Biology, University of Oklahoma , Norman, OK, USA

4. School of Life Sciences, Anhui University , Hefei 230601, PR China

5. Institutes of Material Science and Information Technology, Anhui University , Hefei 230601, PR China

6. Ministry of Education Key Laboratory of Cell Activities and Stress Adaptations, School of Life Sciences, Lanzhou University , Lanzhou 730000, PR China

7. Department of Microbiology and Plant Biology, University of Oklahoma , Norman, OK, USA

8. School of computer science, University of Oklahoma , Norman, OK, USA

9. School of Civil Engineering and Environmental Sciences, University of Oklahoma , Norman, OK, USA

10. Earth and Environmental Sciences, Lawrence Berkeley National Laboratory , Berkeley, CA, USA

Abstract

Abstract Carbohydrate utilization is critical to microbial survival. The phosphotransferase system (PTS) is a well-documented microbial system with a prominent role in carbohydrate metabolism, which can transport carbohydrates through forming a phosphorylation cascade and regulate metabolism by protein phosphorylation or interactions in model strains. However, those PTS-mediated regulated mechanisms have been underexplored in non-model prokaryotes. Here, we performed massive genome mining for PTS components in nearly 15,000 prokaryotic genomes from 4,293 species and revealed a high prevalence of incomplete PTSs in prokaryotes with no association to microbial phylogeny. Among these incomplete PTS carriers, a group of lignocellulose degrading clostridia was identified to have lost PTS sugar transporters and carry a substitution of the conserved histidine residue in the core PTS component, HPr (histidine-phosphorylatable phosphocarrier). Ruminiclostridium cellulolyticum was then selected as a representative to interrogate the function of incomplete PTS components in carbohydrate metabolism. Inactivation of the HPr homolog reduced rather than increased carbohydrate utilization as previously indicated. In addition to regulating distinct transcriptional profiles, PTS associated CcpA (Catabolite Control Protein A) homologs diverged from previously described CcpA with varied metabolic relevance and distinct DNA binding motifs. Furthermore, the DNA binding of CcpA homologs is independent of HPr homolog, which is determined by structural changes at the interface of CcpA homologs, rather than in HPr homolog. These data concordantly support functional and structural diversification of PTS components in metabolic regulation and bring novel understanding of regulatory mechanisms of incomplete PTSs in cellulose-degrading clostridia.

Funder

University of Oklahoma

National Natural Science Foundation of China

Anhui Science and Technology Department

Publisher

Oxford University Press (OUP)

Subject

Ecology, Evolution, Behavior and Systematics,Microbiology

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