Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATP

Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATP

Prokaryote mobilome genomes rely on host machineries for survival and replication. Given that mobile genetic elements (MGEs) derive their energy from host cells, we investigated the diversity of ATP-utilizing proteins in MGE genomes to determine whether they might be associated with proteins that co...

Full description

Bibliographic Details
Main Authors: Hyunjin Shim, Haridha Shivram, Shufei Lei, Jennifer A. Doudna, Jillian F. Banfield
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-07-01
Series:Frontiers in Microbiology
Subjects:
ATPase protein
metagenome
mobilome
host energy
genome editing
antibiotic
Online Access:https://www.frontiersin.org/articles/10.3389/fmicb.2021.691847/full
id doaj-710c5ee8d7da4bf6ac1c69c224601759
record_format Article
spelling doaj-710c5ee8d7da4bf6ac1c69c2246017592021-07-08T11:34:22ZengFrontiers Media S.A.Frontiers in Microbiology1664-302X2021-07-011210.3389/fmicb.2021.691847691847Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATPHyunjin Shim0Haridha Shivram1Shufei Lei2Jennifer A. Doudna3Jillian F. Banfield4Jillian F. Banfield5Jillian F. Banfield6Jillian F. Banfield7Jillian F. Banfield8Jillian F. Banfield9Department of Earth and Planetary Science, University of California, Berkeley, Berkeley, CA, United StatesInnovative Genomics Institute, University of California, Berkeley, Berkeley, CA, United StatesDepartment of Earth and Planetary Science, University of California, Berkeley, Berkeley, CA, United StatesInnovative Genomics Institute, University of California, Berkeley, Berkeley, CA, United StatesDepartment of Earth and Planetary Science, University of California, Berkeley, Berkeley, CA, United StatesInnovative Genomics Institute, University of California, Berkeley, Berkeley, CA, United StatesDepartment of Environmental Science, Policy, and Management, University of California, Berkeley, Berkeley, CA, United StatesEarth Sciences Division, Lawrence Berkeley National Laboratory, Berkeley, CA, United StatesChan Zuckerberg Biohub, San Francisco, CA, United StatesSchool of Earth Sciences, University of Melbourne, Melbourne, VIC, AustraliaProkaryote mobilome genomes rely on host machineries for survival and replication. Given that mobile genetic elements (MGEs) derive their energy from host cells, we investigated the diversity of ATP-utilizing proteins in MGE genomes to determine whether they might be associated with proteins that could suppress related host proteins that consume energy. A comprehensive search of 353 huge phage genomes revealed that up to 9% of the proteins have ATPase domains. For example, ATPase proteins constitute ∼3% of the genomes of Lak phages with ∼550 kbp genomes that occur in the microbiomes of humans and other animals. Statistical analysis shows the number of ATPase proteins increases linearly with genome length, consistent with a large sink for host ATP during replication of megaphages. Using metagenomic data from diverse environments, we found 505 mobilome proteins with ATPase domains fused to diverse functional domains. Among these composite ATPase proteins, 61.6% have known functional domains that could contribute to host energy diversion during the mobilome infection cycle. As many have domains that are known to interact with nucleic acids and proteins, we infer that numerous ATPase proteins are used during replication and for protection from host immune systems. We found a set of uncharacterized ATPase proteins with nuclease and protease activities, displaying unique domain architectures that are energy intensive based on the presence of multiple ATPase domains. In many cases, these composite ATPase proteins genomically co-localize with small proteins in genomic contexts that are reminiscent of toxin-antitoxin systems and phage helicase-antibacterial helicase systems. Small proteins that function as inhibitors may be a common strategy for control of cellular processes, thus could inspire future biochemical experiments for the development of new nucleic acid and protein manipulation tools, with diverse biotechnological applications.https://www.frontiersin.org/articles/10.3389/fmicb.2021.691847/fullATPase proteinmetagenomemobilomehost energygenome editingantibiotic
collection DOAJ
language English
format Article
sources DOAJ
author Hyunjin Shim
Haridha Shivram
Shufei Lei
Jennifer A. Doudna
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
spellingShingle Hyunjin Shim
Haridha Shivram
Shufei Lei
Jennifer A. Doudna
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATP
Frontiers in Microbiology
ATPase protein
metagenome
mobilome
host energy
genome editing
antibiotic
author_facet Hyunjin Shim
Haridha Shivram
Shufei Lei
Jennifer A. Doudna
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
Jillian F. Banfield
author_sort Hyunjin Shim
title Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATP
title_short Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATP
title_full Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATP
title_fullStr Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATP
title_full_unstemmed Diverse ATPase Proteins in Mobilomes Constitute a Large Potential Sink for Prokaryotic Host ATP
title_sort diverse atpase proteins in mobilomes constitute a large potential sink for prokaryotic host atp
publisher Frontiers Media S.A.
series Frontiers in Microbiology
issn 1664-302X
publishDate 2021-07-01
description Prokaryote mobilome genomes rely on host machineries for survival and replication. Given that mobile genetic elements (MGEs) derive their energy from host cells, we investigated the diversity of ATP-utilizing proteins in MGE genomes to determine whether they might be associated with proteins that could suppress related host proteins that consume energy. A comprehensive search of 353 huge phage genomes revealed that up to 9% of the proteins have ATPase domains. For example, ATPase proteins constitute ∼3% of the genomes of Lak phages with ∼550 kbp genomes that occur in the microbiomes of humans and other animals. Statistical analysis shows the number of ATPase proteins increases linearly with genome length, consistent with a large sink for host ATP during replication of megaphages. Using metagenomic data from diverse environments, we found 505 mobilome proteins with ATPase domains fused to diverse functional domains. Among these composite ATPase proteins, 61.6% have known functional domains that could contribute to host energy diversion during the mobilome infection cycle. As many have domains that are known to interact with nucleic acids and proteins, we infer that numerous ATPase proteins are used during replication and for protection from host immune systems. We found a set of uncharacterized ATPase proteins with nuclease and protease activities, displaying unique domain architectures that are energy intensive based on the presence of multiple ATPase domains. In many cases, these composite ATPase proteins genomically co-localize with small proteins in genomic contexts that are reminiscent of toxin-antitoxin systems and phage helicase-antibacterial helicase systems. Small proteins that function as inhibitors may be a common strategy for control of cellular processes, thus could inspire future biochemical experiments for the development of new nucleic acid and protein manipulation tools, with diverse biotechnological applications.
topic ATPase protein
metagenome
mobilome
host energy
genome editing
antibiotic
url https://www.frontiersin.org/articles/10.3389/fmicb.2021.691847/full
work_keys_str_mv AT hyunjinshim diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT haridhashivram diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT shufeilei diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT jenniferadoudna diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT jillianfbanfield diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT jillianfbanfield diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT jillianfbanfield diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT jillianfbanfield diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT jillianfbanfield diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
AT jillianfbanfield diverseatpaseproteinsinmobilomesconstitutealargepotentialsinkforprokaryotichostatp
_version_ 1721313440374456320

Similar Items