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Discovery of an O-mannosylation pathway selectively serving cadherins and protocadherins
by
Vakhrushev, Sergey Y.
, Larsen, Ida Signe Bohse
, Brasch, Julia
, Harrison, Oliver J.
, Siukstaite, Lina
, Goodman, Kerry M.
, Narimatsu, Yoshiki
, Halim, Adnan
, Honig, Barry
, Joshi, Hiren Jitendra
, Hansen, Lars
, Clausen, Henrik
, Shapiro, Lawrence
in
BASIC BIOLOGICAL SCIENCES
/ Biological Sciences
/ Cadherins
/ Cell Biology
/ CRISPR
/ Dolichyl-phosphate-mannose-protein mannosyltransferase
/ Dystroglycan
/ Elongation
/ Enzymes
/ Eukaryotes
/ Evolutionary conservation
/ gene editing
/ Genes
/ glycoproteomics
/ Glycosylation
/ glycosyltransferase
/ Hepatocyte growth factor
/ Homology
/ Lissencephaly
/ Machinery and equipment
/ Mannose
/ mass spectrometry
/ O-glycosylation
/ Polysaccharides
/ Protein synthesis
/ Protocadherin
/ Strands
2017
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Discovery of an O-mannosylation pathway selectively serving cadherins and protocadherins
by
Vakhrushev, Sergey Y.
, Larsen, Ida Signe Bohse
, Brasch, Julia
, Harrison, Oliver J.
, Siukstaite, Lina
, Goodman, Kerry M.
, Narimatsu, Yoshiki
, Halim, Adnan
, Honig, Barry
, Joshi, Hiren Jitendra
, Hansen, Lars
, Clausen, Henrik
, Shapiro, Lawrence
in
BASIC BIOLOGICAL SCIENCES
/ Biological Sciences
/ Cadherins
/ Cell Biology
/ CRISPR
/ Dolichyl-phosphate-mannose-protein mannosyltransferase
/ Dystroglycan
/ Elongation
/ Enzymes
/ Eukaryotes
/ Evolutionary conservation
/ gene editing
/ Genes
/ glycoproteomics
/ Glycosylation
/ glycosyltransferase
/ Hepatocyte growth factor
/ Homology
/ Lissencephaly
/ Machinery and equipment
/ Mannose
/ mass spectrometry
/ O-glycosylation
/ Polysaccharides
/ Protein synthesis
/ Protocadherin
/ Strands
2017
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Discovery of an O-mannosylation pathway selectively serving cadherins and protocadherins
by
Vakhrushev, Sergey Y.
, Larsen, Ida Signe Bohse
, Brasch, Julia
, Harrison, Oliver J.
, Siukstaite, Lina
, Goodman, Kerry M.
, Narimatsu, Yoshiki
, Halim, Adnan
, Honig, Barry
, Joshi, Hiren Jitendra
, Hansen, Lars
, Clausen, Henrik
, Shapiro, Lawrence
in
BASIC BIOLOGICAL SCIENCES
/ Biological Sciences
/ Cadherins
/ Cell Biology
/ CRISPR
/ Dolichyl-phosphate-mannose-protein mannosyltransferase
/ Dystroglycan
/ Elongation
/ Enzymes
/ Eukaryotes
/ Evolutionary conservation
/ gene editing
/ Genes
/ glycoproteomics
/ Glycosylation
/ glycosyltransferase
/ Hepatocyte growth factor
/ Homology
/ Lissencephaly
/ Machinery and equipment
/ Mannose
/ mass spectrometry
/ O-glycosylation
/ Polysaccharides
/ Protein synthesis
/ Protocadherin
/ Strands
2017
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Discovery of an O-mannosylation pathway selectively serving cadherins and protocadherins
Journal Article
Discovery of an O-mannosylation pathway selectively serving cadherins and protocadherins
2017
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Overview
The cadherin (cdh) superfamily of adhesion molecules carry O-linked mannose (O-Man) glycans at highly conserved sites localized to specific β-strands of their extracellular cdh (EC) domains. These O-Man glycans do not appear to be elongated like O-Man glycans found on α-dystroglycan (α-DG), and we recently demonstrated that initiation of cdh/protocadherin (pcdh) O-Man glycosylation is not dependent on the evolutionary conserved POMT1/POMT2 enzymes that initiate O-Man glycosylation on α-DG. Here, we used a CRISPR/Cas9 genetic dissection strategy combined with sensitive and quantitative O-Man glycoproteomics to identify a homologous family of four putative protein O-mannosyltransferases encoded by the TMTC1–4 genes, which were found to be imperative for cdh and pcdh O-Man glycosylation. KO of all four TMTC genes in HEK293 cells resulted in specific loss of cdh and pcdh O-Man glycosylation, whereas combined KO of TMTC1 and TMTC3 resulted in selective loss of O-Man glycans on specific β-strands of EC domains, suggesting that each isoenzyme serves a different function. In addition, O-Man glycosylation of IPT/TIG domains of plexins and hepatocyte growth factor receptor was not affected in TMTC KO cells, suggesting the existence of yet another O-Man glycosylation machinery. Our study demonstrates that regulation of O-mannosylation in higher eukaryotes is more complex than envisioned, and the discovery of the functions of TMTCs provide insight into cobblestone lissencephaly caused by deficiency in TMTC3.
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