Congenital disorders of glycosylation (CDG) comprise a family of human multisystemic diseases caused by recessive mutations in genes required for protein N-glycosylation. More than 100 distinct forms of CDGs have been identified and most of them cause severe neurological impairment. The Conserved Oligomeric Golgi (COG) complexmediates tethering of vesicles carrying glycosylation enzymes across the Golgi cisternae. Mutations affecting human COG1, COG2 and COG4-COG8 cause monogenic forms of inherited, autosomal recessive CDGs.We have generated a Drosophila COG7-CDG model that closely parallels the pathological characteristics of COG7-CDG patients, including pronounced neuromotor defects associated with altered N-glycome profiles. Consistent with these alterations, larval neuromuscular junctions of Cog7 mutants exhibit a significant reduction in bouton numbers. We demonstrate that the COG complex cooperates with Rab1 and Golgi phosphoprotein 3 to regulate Golgi trafficking and that overexpression of Rab1 can rescue the cytokinesis and locomotor defects associated with loss of Cog7. Our results suggest that the Drosophila COG7-CDG model can be used to test novel potential therapeutic strategies by modulating trafficking pathways.

COG7 deficiency in Drosophila generates multifaceted developmental, behavioral and protein glycosylation phenotypes / Frappaolo, A.; Sechi, S.; Kumagai, T.; Robinson, S.; Fraschini, R.; Karimpour-Ghahnavieh, A.; Belloni, G.; Piergentili, R.; Tiemeyer, K. H.; Tiemeyer, M.; Giansanti, M. G.. - In: JOURNAL OF CELL SCIENCE. - ISSN 0021-9533. - 130:21(2017), pp. 3637-3649. [10.1242/jcs.209049]

COG7 deficiency in Drosophila generates multifaceted developmental, behavioral and protein glycosylation phenotypes

Karimpour-Ghahnavieh A.;Belloni G.;Piergentili R.;
2017

Abstract

Congenital disorders of glycosylation (CDG) comprise a family of human multisystemic diseases caused by recessive mutations in genes required for protein N-glycosylation. More than 100 distinct forms of CDGs have been identified and most of them cause severe neurological impairment. The Conserved Oligomeric Golgi (COG) complexmediates tethering of vesicles carrying glycosylation enzymes across the Golgi cisternae. Mutations affecting human COG1, COG2 and COG4-COG8 cause monogenic forms of inherited, autosomal recessive CDGs.We have generated a Drosophila COG7-CDG model that closely parallels the pathological characteristics of COG7-CDG patients, including pronounced neuromotor defects associated with altered N-glycome profiles. Consistent with these alterations, larval neuromuscular junctions of Cog7 mutants exhibit a significant reduction in bouton numbers. We demonstrate that the COG complex cooperates with Rab1 and Golgi phosphoprotein 3 to regulate Golgi trafficking and that overexpression of Rab1 can rescue the cytokinesis and locomotor defects associated with loss of Cog7. Our results suggest that the Drosophila COG7-CDG model can be used to test novel potential therapeutic strategies by modulating trafficking pathways.
2017
COG7; Drosophila; glycosylation; Golgi; GOLPH3; animals; biological transport; congenital disorders of glycosylation; disease models, animal; drosophila proteins; drosophila melanogaster; gait disorders, neurologic; gene deletion; gene xpression egulation, evelopmental; enetic omplementation est; glycosylation; Golgi pparatus; umans; arva; Mannose; euromuscular Junction; ncogene roteins; henotype; olysaccharides; vesicular transport proteins; rab GTP-binding proteins; protein processing, post-translational
01 Pubblicazione su rivista::01a Articolo in rivista
COG7 deficiency in Drosophila generates multifaceted developmental, behavioral and protein glycosylation phenotypes / Frappaolo, A.; Sechi, S.; Kumagai, T.; Robinson, S.; Fraschini, R.; Karimpour-Ghahnavieh, A.; Belloni, G.; Piergentili, R.; Tiemeyer, K. H.; Tiemeyer, M.; Giansanti, M. G.. - In: JOURNAL OF CELL SCIENCE. - ISSN 0021-9533. - 130:21(2017), pp. 3637-3649. [10.1242/jcs.209049]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1394194
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