Glycoproteins traversing the eukaryotic secretory pathway begin life in the endoplasmic reticulum (ER), where their folding is surveyed by the 170-kDa UDP-glucose:glycoprotein glucosyltransferase (UGGT). The enzyme acts as the single glycoprotein folding quality control checkpoint: it selectively reglucosylates misfolded glycoproteins, promotes their association with ER lectins and associated chaperones, and prevents premature secretion from the ER. UGGT has long resisted structural determination and sequence-based domain boundary prediction. Questions remain on how this single enzyme can flag misfolded glycoproteins of different sizes and shapes for ER retention and how it can span variable distances between the site of misfold and a glucose-accepting N-linked glycan on the same glycoprotein. Here, crystal structures of a full-length eukaryotic UGGT reveal four thioredoxin-like (TRXL) domains arranged in a long arc that terminates in two β-sandwiches tightly clasping the glucosyltransferase domain. The fold of the molecule is topologically complex, with the first β-sandwich and the fourth TRXL domain being encoded by nonconsecutive stretches of sequence. In addition to the crystal structures, a 15-Å cryo-EM reconstruction reveals interdomain flexibility of the TRXL domains. Double cysteine point mutants that engineer extra interdomain disulfide bridges rigidify the UGGT structure and exhibit impaired activity. The intrinsic flexibility of the TRXL domains of UGGT may therefore endow the enzyme with the promiscuity needed to recognize and reglucosylate its many different substrates and/or enable reglucosylation of N-linked glycans situated at variable distances from the site of misfold.

Interdomain conformational flexibility underpins the activity of UGGT, the eukaryotic glycoprotein secretion checkpoint / Roversi, Pietro; Marti, Lucia; Caputo, Alessandro T.; Alonzi, Dominic S.; Hill, Johan C.; Dent, Kyle C.; Kumar, Abhinav; Levasseur, Mikail D.; Lia, Andrea; Waksman, Thomas; Basu, Souradeep; Soto Albrecht, Yentli; Qian, Kristin; Mcivor, James Patrick; Lipp, Colette B.; Siliqi, Dritan; Vasiljević, Snežana; Mohammed, Shabaz; Lukacik, Petra; Walsh, Martin A.; Santino, Angelo; Zitzmann, Nicole. - In: PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA. - ISSN 0027-8424. - 114:32(2017), pp. 8544-8549. [10.1073/pnas.1703682114]

Interdomain conformational flexibility underpins the activity of UGGT, the eukaryotic glycoprotein secretion checkpoint

Marti, Lucia
Co-primo
;
2017

Abstract

Glycoproteins traversing the eukaryotic secretory pathway begin life in the endoplasmic reticulum (ER), where their folding is surveyed by the 170-kDa UDP-glucose:glycoprotein glucosyltransferase (UGGT). The enzyme acts as the single glycoprotein folding quality control checkpoint: it selectively reglucosylates misfolded glycoproteins, promotes their association with ER lectins and associated chaperones, and prevents premature secretion from the ER. UGGT has long resisted structural determination and sequence-based domain boundary prediction. Questions remain on how this single enzyme can flag misfolded glycoproteins of different sizes and shapes for ER retention and how it can span variable distances between the site of misfold and a glucose-accepting N-linked glycan on the same glycoprotein. Here, crystal structures of a full-length eukaryotic UGGT reveal four thioredoxin-like (TRXL) domains arranged in a long arc that terminates in two β-sandwiches tightly clasping the glucosyltransferase domain. The fold of the molecule is topologically complex, with the first β-sandwich and the fourth TRXL domain being encoded by nonconsecutive stretches of sequence. In addition to the crystal structures, a 15-Å cryo-EM reconstruction reveals interdomain flexibility of the TRXL domains. Double cysteine point mutants that engineer extra interdomain disulfide bridges rigidify the UGGT structure and exhibit impaired activity. The intrinsic flexibility of the TRXL domains of UGGT may therefore endow the enzyme with the promiscuity needed to recognize and reglucosylate its many different substrates and/or enable reglucosylation of N-linked glycans situated at variable distances from the site of misfold.
2017
Endoplasmic reticulum; Eukaryotic secretion; Glycoprotein folding; UDP-glucose glycoprotein glucosyltransferase; UGGT; Animals; Chaetomium; Crystallography, X-Ray; Endoplasmic Reticulum; Eukaryota; Eukaryotic Cells; Glucosyltransferases; Glycoproteins; Molecular Conformation; Protein Domains; Protein Folding; Protein Transport; Substrate Specificity; Multidisciplinary
01 Pubblicazione su rivista::01a Articolo in rivista
Interdomain conformational flexibility underpins the activity of UGGT, the eukaryotic glycoprotein secretion checkpoint / Roversi, Pietro; Marti, Lucia; Caputo, Alessandro T.; Alonzi, Dominic S.; Hill, Johan C.; Dent, Kyle C.; Kumar, Abhinav; Levasseur, Mikail D.; Lia, Andrea; Waksman, Thomas; Basu, Souradeep; Soto Albrecht, Yentli; Qian, Kristin; Mcivor, James Patrick; Lipp, Colette B.; Siliqi, Dritan; Vasiljević, Snežana; Mohammed, Shabaz; Lukacik, Petra; Walsh, Martin A.; Santino, Angelo; Zitzmann, Nicole. - In: PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA. - ISSN 0027-8424. - 114:32(2017), pp. 8544-8549. [10.1073/pnas.1703682114]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1118679
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