par Virgilio, Enrico 
;Tielens, Sylvia;Bonfield, Georgia;Nian, Fang-Shin;Sawatani, Toshiaki ;Vinci, Chiara ;Govier, Molly;Montaser, Hossam El-dien ;Lartigue, Romane;Arunagiri, Anoop;Liboz, Alexandrine ;Natividade da Silva, Flávia ;Lytrivi, Maria ;Papadopoulou, Theodora ;Wakeling, Matthew Neil;Russ-Silsby, James;Bowman, Pamela;Johnson, Matthew B;Laver, Thomas W;Piron, Anthony ;Yi, Xiaoyan ;Fantuzzi, Federica ;Hendrickx, Sirine;Igoillo Esteve, Mariana ;Santacreu, Bruno Jaime ;Suntharesan, Jananie;Ghildiyal, Radha;Hegde, Darshan DG;Shah, Nikhil Avnish;Acar, Sezer;Özkaya Dönmez, Beyhan;Özkan, Behzat;Mohsin, Fauzia;Talaat, Iman IM;Abbas, Mohamed Tarek;Abbas, Omar Saied;Alghamdi, Hamed Ali;Kandemir, Nurgun;Flanagan, Sarah E.;Scharfmann, Raphaël;Arvan, Peter;Raoux, Matthieu;Nguyen, Laurent;Hattersley, Andrew T;Cnop, Miriam ;De Franco, Elisa
Référence The Journal of clinical investigation
Publication Publié, 2025-09-01
;Tielens, Sylvia;Bonfield, Georgia;Nian, Fang-Shin;Sawatani, Toshiaki ;Vinci, Chiara ;Govier, Molly;Montaser, Hossam El-dien ;Lartigue, Romane;Arunagiri, Anoop;Liboz, Alexandrine ;Natividade da Silva, Flávia ;Lytrivi, Maria ;Papadopoulou, Theodora ;Wakeling, Matthew Neil;Russ-Silsby, James;Bowman, Pamela;Johnson, Matthew B;Laver, Thomas W;Piron, Anthony ;Yi, Xiaoyan ;Fantuzzi, Federica ;Hendrickx, Sirine;Igoillo Esteve, Mariana ;Santacreu, Bruno Jaime ;Suntharesan, Jananie;Ghildiyal, Radha;Hegde, Darshan DG;Shah, Nikhil Avnish;Acar, Sezer;Özkaya Dönmez, Beyhan;Özkan, Behzat;Mohsin, Fauzia;Talaat, Iman IM;Abbas, Mohamed Tarek;Abbas, Omar Saied;Alghamdi, Hamed Ali;Kandemir, Nurgun;Flanagan, Sarah E.;Scharfmann, Raphaël;Arvan, Peter;Raoux, Matthieu;Nguyen, Laurent;Hattersley, Andrew T;Cnop, Miriam ;De Franco, ElisaRéférence The Journal of clinical investigation
Publication Publié, 2025-09-01
Article révisé par les pairs
| Résumé : | Understanding the genetic causes of diseases affecting pancreatic β cells and neurons can give insights into pathways essential for both cell types. Microcephaly, epilepsy and diabetes syndrome (MEDS) is a congenital disorder with two known aetiological genes, IER3IP1 and YIPF5. Both genes encode proteins involved in endoplasmic reticulum (ER) to Golgi trafficking. We used genome sequencing to identify 6 individuals with MEDS caused by biallelic variants in the novel disease gene, TMEM167A. All had neonatal diabetes (diagnosed <6 months) and severe microcephaly, five also had epilepsy. TMEM167A is highly expressed in developing and adult human pancreas and brain. To gain insights into the mechanisms leading to diabetes, we silenced TMEM167A in EndoC-βH1 cells and knocked-in one patient's variant, p.Val59Glu, in induced pluripotent stem cells (iPSCs). Both TMEM167A depletion in EndoC-βH1 cells and the p.Val59Glu variant in iPSC-derived β cells sensitized β cells to ER stress. The p.Val59Glu variant impaired proinsulin trafficking to the Golgi and induced iPSC-β cell dysfunction. The discovery of TMEM167A variants as a new genetic cause of MEDS highlights a critical role of TMEM167A in the ER to Golgi pathway in β cells and neurons. |
