Type IV The Type IV Secretion System
T4SS is found in many species of Gram-negative and Gram-positive
bacteria as well as in
archea and are typically associated with conjugation or delivery of virulence proteins to eukaryotic cells. Some species of plant pathogen
Xanthomonas, however, possess a particular T4SS capable of mediating CDI by delivering a peptidoglycan hydrolase. This effector kills targets that do not have the cognate immunity protein similar to other CDI systems.
Type V The first CDI system to be discovered was a Type V secretion system, encoded by the
cdiBAI gene cluster found widespread throughout pathogenic Gram-negative bacteria. The first protein encoded in the operon, CdiB, is an outer membrane
beta-barrel protein that exports CdiA, presenting it on the cell surface of a CDI-expressing (CDI+) bacterium. CdiA is predicted to form a filament several nanometers long that extends outward from the CDI+ cell in order to interact with neighbouring bacteria via outer membrane protein receptors to which it will bind. CdiI is an immunity protein to prevent auto-inhibition by the C-terminal toxin. This also prevents the bacteria from killing or inhibiting the growth of their siblings as long as these possess the immunity gene. Many CDI systems contain additional pairs called "orphans" following the first copy and these orphans can be connected to different main CdiA:s in a modular fashion. The T6SS is capable of delivering effectors to both
prokaryote and
eukaryotes target cells. Upon contraction of the T6SS, effectors are transported across the cytosol of the bacteria cell into the target cells. Effectors are loaded onto this dynamic secretion system through interactions with Hcp, VgrG and PAAR-domains. The full list of T6SS effectors is not known.
Rhs toxins The Rearrangement hotspot system (Rhs) exists in both Gram-negative and
Gram-positive bacteria. Similar to CdiA, these systems consists of big proteins with a conserved
N-terminal domain and a variable C-terminal toxin domain requiring a cognate immunity protein. Many Rhs systems contain PAAR-domains (Proline-Alanine-Alanine-Arginine) which can interact with the VgrG of the T6SS apparatus making it required for Rhs secretion. The name Rearrangement hotspots comes from the discovery when the system was first identified as elements on the
E. coli chromosome that were continuously
rearranging. The Gram-positive soil bacterium
Bacillus subtilis possesses an Rhs homolog called Wall-associated protein A (WapA) capable of mediating CDI whilst requiring a cognate immunity protein, WapI, to prevent auto-inhibition. == Other functions ==