功能缺陷型UBOX5变体与原发性闭角型青光眼
Functionally deficient UBOX5 variants and primary angle-closure glaucoma.
作者信息
Li Zheng, Chng Wee Ling, Liu Zhehao, Do Tan, Nakano Masakazu, Chen Li Jia, Loo Yunhua, Chan Anita S Y, Topouzis Fotis, Nongpiur Monisha E, Ozaki Mineo, Nakano Satoko, Kubota Toshiaki, Perera Shamira A, Husain Rahat, Wong Tina T L, Cheng Ching-Yu, Ho Ching Lin, Abu-Amero Khaled, Wong Hon-Tym, Melo Mônica Barbosa de, Hien Nguyen Do Thi Ngoc, Van Trinh Nguyen, Huong Nguyen Thi Thanh, Azhany Yaakub, Perez-Grossmann Rodolfo, Chan Poemen Pm, Stuart Kelsey V, Biradar Mahantesh I, Szabo Anita, Anastasopoulos Eleftherios, Giannoulis Dimitrios A, Ntonti Panagiota, Papakonstantinou Evangelia, Lambropoulos Alexandros, Chatzikyriakidou Anthoula, Kilintzis Vassilis, Ayub Humaira, Micheal Shazia, Aung Yee Yee, Leuenberger Edgar U, Fea Antonio, Mon Naing Naing, Anajao Amihan, Bi Xuezhi, Kok Yee Jiun, Chong Rachel S, Boey Pui-Yi, Tan Darrell Zi Jing, Sin Wendy Wan Ling, Chowbay Balram, Khaing Chaw Chaw, Aung Yin Mon, Reyes Rigo Daniel, Panagiotou Evangelia S, Mikropoulos Dimitrios G, Voudouragkaki Irini C, Panos Georgios D, Xie Zhicheng, Chen Xiao Yin, Lim Yi Ting, Meah Wee Yang, Lee Ying Shi, Ho Candice Ee Hua, Yeo Pearlyn Mei Xin, Ikeda Yoko, Tokuda Yuichi, Tanaka Masami, Omi Natsue, Ueno Morio, de Vasconcellos José P C, Costa Vital P, Abe Ricardo Y, de Souza Bruno B, Fong Guillermo B, Castro Vania V, Fujita Ricardo, Guevara-Fujita Maria L, Akhtar Farah, Ali Mahmood, Catacutan Mary Ann T, Felarca Irene R, Liao Chona S, Lavia Carlo, Than Hlaing May, Oo Khin Thida, Soe-Kyaw Phyu P, Frezzotti Paolo, Pasutto Francesca, Quino Raquel, Minn-Din Zaw, Oo Nay Lin, Dallorto Laura, Set Saw Htoo, Doan Vi Huyen, Qamar Raheel, Neto Jamil Miguel, Al-Obeidan Saleh, Tham Clement C, Mori Kazuhiko, Sotozono Chie, Kinoshita Shigeru, Konstas Anastasios G, Liza-Sharmini Ahmad Tajudin, Zenteno Juan C, Do Nhu Hon, Foster Paul J, Tashiro Kei, Pang Chi Pui, Khawaja Anthony P, Aung Tin, Wang Zhenxun, Khor Chiea Chuen
机构信息
Genome Institute of Singapore (GIS), Agency for Science, Technology and Research (A*STAR), 60 Biopolis Street, Genome #02-01, Singapore, 138672, Republic of Singapore.
Duke-NUS Medical School, National University of, Singapore, Singapore.
出版信息
Nat Commun. 2025 Aug 15;16(1):7620. doi: 10.1038/s41467-025-62775-x.
Primary angle-closure glaucoma is a major cause of irreversible blindness worldwide afflicting >20 million people. Through whole exome sequencing, we analysed the association between gene-based burden of rare, protein-altering genetic variants and disease risk in 4,667 affected individuals and 5,473 unaffected controls. We tested genes surpassing exome-wide significance (P < 2.5 × 10) for replication in a further 2,519 cases and 472,189 controls. We observed carriers of rare, protein-altering variants at UBOX5 (observed in 154 out of 7,186 affected individuals [2.1%] and in 3,975 out of 477,197 unaffected controls [0.83%]) to be associated with 2.13-fold increased risk of PACG (95%ci, 1.69 - 2.69; P = 1.25 × 10). We performed substrate trapping assays coupled with mass spectrometry and observed Binding Immunoglobulin Protein (BIP) as a key substrate for UBOX5. Biological assays showed UBOX5 acts by ubiquitinating BIP. We evaluated the functional status of 35 UBOX5 variants and observed that functionally deficient variants were enriched in affected individuals compared to controls. We validated this finding in an independent collection where 3 persons carrying functionally deficient variants were observed out of 208 cases (1.4%), whereas none were observed in 600 controls. Our findings suggest the UBOX5-BIP signalling pathway might be involved in biology of primary angle-closure glaucoma.
原发性闭角型青光眼是全球不可逆失明的主要原因,影响着超过2000万人。通过全外显子组测序,我们分析了4667名患者和5473名对照中罕见的、导致蛋白质改变的基因变异的基因负担与疾病风险之间的关联。我们对超过外显子组水平显著性(P < 2.5×10)的基因在另外2519例患者和472189名对照中进行了验证。我们观察到UBOX5基因中罕见的、导致蛋白质改变的变异携带者(在7186名患者中有154名[2.1%],在477197名对照中有3975名[0.83%])与原发性闭角型青光眼风险增加2.13倍相关(95%可信区间,1.69 - 2.69;P = 1.25×10)。我们进行了底物捕获分析并结合质谱分析,观察到结合免疫球蛋白蛋白(BIP)是UBOX5的关键底物。生物学分析表明UBOX5通过泛素化BIP发挥作用。我们评估了35种UBOX5变异的功能状态,观察到与对照相比,功能缺陷型变异在患者中更为富集。我们在一个独立队列中验证了这一发现,在208例患者中有3例(1.4%)携带功能缺陷型变异,而在600名对照中未观察到。我们的研究结果表明,UBOX5 - BIP信号通路可能参与原发性闭角型青光眼的生物学过程。
Zotero 插件