The TisB-IstR toxin-antitoxin system is the first known

toxin-antitoxin system A toxin-antitoxin system is a set of two or more closely linked genes that together encode both a "toxin" protein and a corresponding "antitoxin". Toxin-antitoxin systems are widely distributed in prokaryotes, and organisms often have them in mul ...

which is induced by the

SOS response The SOS response is a global response to DNA damage in which the cell cycle is arrested and DNA repair and mutagenesis is induced. The system involves the RecA protein ( Rad51 in eukaryotes). The RecA protein, stimulated by single-stranded D ...

in response to DNA damage.

IstR-1 and IstR-2

IstR sRNA (inhibitor of SOS-induced toxicity by RNA) is a family of non-coding RNA first identified in ''

Escherichia coli ''Escherichia coli'' (),Wells, J. C. (2000) Longman Pronunciation Dictionary. Harlow ngland Pearson Education Ltd. also known as ''E. coli'' (), is a Gram-negative, facultative anaerobic, rod-shaped, coliform bacterium of the genus '' Esc ...

''. There are two small RNAs encoded by the IstR locus: IstR-1 and IstR-2, of which IstR-1 works as antitoxins against the toxic

protein Proteins are large biomolecules and macromolecules that comprise one or more long chains of amino acid residues. Proteins perform a vast array of functions within organisms, including catalysing metabolic reactions, DNA replication, respon ...

br>TisB
(toxicity-induced by SOS B) which is encoded by the neighbouring ''tisAB''

gene In biology, the word gene (from , ; "... Wilhelm Johannsen coined the word gene to describe the Mendelian units of heredity..." meaning ''generation'' or ''birth'' or ''gender'') can have several different meanings. The Mendelian gene is a b ...

. IstR-1 is a 75 nucleotide transcript expressed constitutively throughout growth, whereas IstR-2 is a 140 nucleotide transcript induced by Mitomycin C (MMC). Both IstR-2 and ''tisAB'' are thought to be regulated by LexA while IstR-1 is constitutively transcribed.

Deletion Deletion or delete may refer to: Computing * File deletion, a way of removing a file from a computer's file system * Code cleanup, a way of removing unnecessary variables, data structures, cookies, and temporary files in a programming language * ...

analysis confirmed the function of IstR, ''E. coli'' strain K-12 could not grow in the absence of IstR when ''tisAB'' was present. Inserting IstR genes on a

plasmid A plasmid is a small, extrachromosomal DNA molecule within a cell that is physically separated from chromosomal DNA and can replicate independently. They are most commonly found as small circular, double-stranded DNA molecules in bacteria; howev ...

allowed the bacteria to grow normally. Further studies showed that expression of IstR-1 alone is enough to remedy the toxic effects of TisB. IstR-2 is not involved in the regulation of ''tisAB''.

''TisAB''

The ''tisAB'' locus codes for two genes: ''tisA'' and ''tisB''. The ''tisA'' reading frame was shown through a translation assay to not be translated. Its sequence is unconserved across species. TisB is a 29 amino acid peptide widely conserved in enterobacteria. TisB is responsible for conferring toxicity through suspected

membrane A membrane is a selective barrier; it allows some things to pass through but stops others. Such things may be molecules, ions, or other small particles. Membranes can be generally classified into synthetic membranes and biological membranes. ...

disruption. Upon translation of the ''tisB'' gene, a +1 inactive primary transcript mRNA is produced, which must be endonucleolytically processed 42 nucleotides from the 5' end to yield a +42 translationally competent mRNA. In the +42 form, the mRNA has a ribosome loading/standby site in an unstructured region >80 nt upstream of the ''tisB'' ribosome binding site, thus allowing translation of the TisB protein. This standby site is structurally unavailable in the inactive forms of the ''tisB'' mRNA (the +1 form and the +106 form produced by RNase III cleavage).

Mechanism of TisB inhibition by IstR-1

IstR-1 is thought to both inhibit translation of the TisB toxin, and promote RNase III cleavage of the RNA duplex formed when IstR-1 base pairs to ''tisB'' mRNA. Binding of the complementary sequence of ''istR-1'' sRNA to ''tisB'' mRNA in the ribosome standby site is thought to prevent loading of ribosomes and therefore prevent translation of the TisB protein. A RACE analysis confirmed that IstR-1 binds TisB

mRNA In molecular biology, messenger ribonucleic acid (mRNA) is a single-stranded molecule of RNA that corresponds to the genetic sequence of a gene, and is read by a ribosome in the process of synthesizing a protein. mRNA is created during the ...

and the duplex is then degraded by RNase III. Degradation results in a +106 form, an inactive 249 nt transcript which cannot be translated.

Proposed function of the IstR-TisB toxin-antitoxin system

The proposed function of this

is to cause growth arrest, rather than cell death, in response to DNA damage, allowing time for repair processes to occur. TisB translation is under LexA control, so it is induced by DNA damage as part of the

. Under normal conditions, very little ''tisB'' mRNA is synthesised and translation is inhibited, but when DNA damage occurs ''tisAB'' is strongly induced causing overexpression, which overrides inhibition by depleting the IstR-1 pool. Experimental data has shown effects of TisB to be decreases in transcription, translation and replication, RNA degradation and ribosome disassembly. TisB does not affect transcription and translation directly ''in vitro'', so these effects are thought to be downstream consequences of membrane damage. TisB insertion into the membrane is thought to result in a loss of membrane potential. This could account for a decrease in ATP concentration in cells following triggering of the SOS response, causing slowing of cellular processes and inhibited cell growth.

References

External links

*
EcoCyc page for Istr-1EcoliWiki page for TisB
{{DEFAULTSORT:Istr Rna Antisense RNA RNA antitoxins Toxins