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The structure of EXTL3 helps to explain the different roles of bi-domain exostosins in heparan sulfate synthesis.


ABSTRACT: Heparan sulfate is a highly modified O-linked glycan that performs diverse physiological roles in animal tissues. Though quickly modified, it is initially synthesised as a polysaccharide of alternating β-D-glucuronosyl and N-acetyl-α-D-glucosaminyl residues by exostosins. These enzymes generally possess two glycosyltransferase domains (GT47 and GT64)-each thought to add one type of monosaccharide unit to the backbone. Although previous structures of murine exostosin-like 2 (EXTL2) provide insight into the GT64 domain, the rest of the bi-domain architecture is yet to be characterised; hence, how the two domains co-operate is unknown. Here, we report the structure of human exostosin-like 3 (EXTL3) in apo and UDP-bound forms. We explain the ineffectiveness of EXTL3's GT47 domain to transfer β-D-glucuronosyl units, and we observe that, in general, the bi-domain architecture would preclude a processive mechanism of backbone extension. We therefore propose that heparan sulfate backbone polymerisation occurs by a simple dissociative mechanism.

SUBMITTER: Wilson LFL 

PROVIDER: S-EPMC9178029 | biostudies-literature | 2022 Jun

REPOSITORIES: biostudies-literature

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The structure of EXTL3 helps to explain the different roles of bi-domain exostosins in heparan sulfate synthesis.

Wilson L F L LFL   Dendooven T T   Hardwick S W SW   Echevarría-Poza A A   Tryfona T T   Krogh K B R M KBRM   Chirgadze D Y DY   Luisi B F BF   Logan D T DT   Mani K K   Dupree P P  

Nature communications 20220608 1


Heparan sulfate is a highly modified O-linked glycan that performs diverse physiological roles in animal tissues. Though quickly modified, it is initially synthesised as a polysaccharide of alternating β-D-glucuronosyl and N-acetyl-α-D-glucosaminyl residues by exostosins. These enzymes generally possess two glycosyltransferase domains (GT47 and GT64)-each thought to add one type of monosaccharide unit to the backbone. Although previous structures of murine exostosin-like 2 (EXTL2) provide insigh  ...[more]

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