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PilZ domain
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The PilZ family is named after the type IV pilus control protein first identified in Pseudomonas aeruginosa, expressed as part of the pil . It has a location and is essential for type IV fimbrial, or pilus, . PilZ is a c-di-GMP domain and PilZ domain-containing proteins represent the best studied class of c-di-GMP effectors. C-di-GMP, cyclic diguanosine monophosphate, the second messenger in cells, is widespread in and unique to the bacterial kingdom. Elevated levels of c-di-GMP generally cause bacteria to change from a single-cell state to a sessile, adhesive surface-attached multicellular state called .

Proteins which contain PilZ are known to interact with the flagellar switch-complex proteins FliG and FliM and this is mediated via the c-di-GMP-PliZ complex. This interaction results in a reduction of and induces counterclockwise motor bias that slows the motor and induces counterclockwise rotation, inhibiting .

Binding and mutagenesis studies of several PilZ domain proteins have shown that c-di-GMP binding depends on residues in RxxxR and D/NxSxxG . The crystal structure, at 1.7 A, of a PilZ domain::c-di-GMP complex from shows c-di-GMP contacting seven of nine strongly conserved residues. Binding of c-di-GMP causes a conformational switch whereby the C- and N-terminal domains are brought into close opposition forming a new allosteric interaction surface that spans these domains and the c-di-GMP at their interface.

The PilZ domain is also implicated in the bacterial of the , Borrelia burgdorferi, through its binding partner c-di-GMP.

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