Identifying Small Open Reading Frames in Prokaryotes with Ribosome Profiling

Nora Vazquez-Laslop; Cynthia M. Sharma; Alexander Mankin; Allen R. Buskirk

doi:10.1128/JB.00294-21

Identifying Small Open Reading Frames in Prokaryotes with Ribosome Profiling

Nora Vazquez-Laslop, Cynthia M. Sharma, Alexander Mankin, Allen R. Buskirk

School of Medicine

Research output: Contribution to journal › Article › peer-review

Abstract

Small proteins encoded by open reading frames (ORFs) shorter than 50 codons (small ORFs [sORFs]) are often overlooked by annotation engines and are difficult to characterize using traditional biochemical techniques. Ribosome profiling has tremendous potential to empirically improve the annotations of prokaryotic genomes. Recent improvements in ribosome profiling methods for bacterial model organisms have revealed many new sORFs in well-characterized genomes. Antibiotics that trap ribosomes just after initiation have played a key role in these developments by allowing the unambiguous identification of the start codons (and, hence, the reading frame) for novel ORFs. Here, we describe these new methods and highlight critical controls and considerations for adapting ribosome profiling to different prokaryotic species.

Original language	English (US)
Article number	e00294-21
Journal	Journal of bacteriology
Volume	204
Issue number	1
DOIs	https://doi.org/10.1128/JB.00294-21
State	Published - Jan 2022

Keywords

Genome annotation
Ribosome profiling
SORF
Small protein

ASJC Scopus subject areas

Molecular Biology
Microbiology

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10.1128/JB.00294-21

Cite this

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title = "Identifying Small Open Reading Frames in Prokaryotes with Ribosome Profiling",

abstract = "Small proteins encoded by open reading frames (ORFs) shorter than 50 codons (small ORFs [sORFs]) are often overlooked by annotation engines and are difficult to characterize using traditional biochemical techniques. Ribosome profiling has tremendous potential to empirically improve the annotations of prokaryotic genomes. Recent improvements in ribosome profiling methods for bacterial model organisms have revealed many new sORFs in well-characterized genomes. Antibiotics that trap ribosomes just after initiation have played a key role in these developments by allowing the unambiguous identification of the start codons (and, hence, the reading frame) for novel ORFs. Here, we describe these new methods and highlight critical controls and considerations for adapting ribosome profiling to different prokaryotic species.",

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AU - Mankin, Alexander

AU - Buskirk, Allen R.

PY - 2022/1

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AB - Small proteins encoded by open reading frames (ORFs) shorter than 50 codons (small ORFs [sORFs]) are often overlooked by annotation engines and are difficult to characterize using traditional biochemical techniques. Ribosome profiling has tremendous potential to empirically improve the annotations of prokaryotic genomes. Recent improvements in ribosome profiling methods for bacterial model organisms have revealed many new sORFs in well-characterized genomes. Antibiotics that trap ribosomes just after initiation have played a key role in these developments by allowing the unambiguous identification of the start codons (and, hence, the reading frame) for novel ORFs. Here, we describe these new methods and highlight critical controls and considerations for adapting ribosome profiling to different prokaryotic species.

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KW - Small protein

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Identifying Small Open Reading Frames in Prokaryotes with Ribosome Profiling

Abstract

Keywords

ASJC Scopus subject areas

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