Your search keyword '"Butt, Taeed A."' showing total 2 results

1. High morbidity and mortality in children with untreated congenital deficiency of leptin or its receptor

Author

Saeed, Sadia, Khanam, Roohia, Janjua, Qasim M., Manzoor, Jaida, Ning, Lijiao, Hanook, Sharoon, Canouil, Mickaël, Ali, Muhammad, Ayesha, Hina, Khan, Waqas I., Farooqi, I. Sadaf, Yeo, Giles S.H., O'Rahilly, Stephen, Bonnefond, Amélie, Butt, Taeed A., Arslan, Muhammad, and Froguel, Philippe

Abstract

The long-term clinical outcomes of severe obesity due to leptin signaling deficiency are unknown. We carry out a retrospective cross-sectional investigation of a large cohort of children with leptin (LEP), LEP receptor (LEPR), or melanocortin 4 receptor (MC4R) deficiency (n = 145) to evaluate the progression of the disease. The affected individuals undergo physical, clinical, and metabolic evaluations. We report a very high mortality in children with LEP (26%) or LEPR deficiency (9%), mainly due to severe pulmonary and gastrointestinal infections. In addition, 40% of surviving children with LEP or LEPR deficiency experience life-threatening episodes of lung or gastrointestinal infections. Although precision drugs are currently available for LEP and LEPR deficiencies, as yet, they are not accessible in Pakistan. An appreciation of the severe impact of LEP or LEPR deficiency on morbidity and early mortality, educational attainment, and the attendant stigmatization should spur efforts to deliver the available life-saving drugs to these children as a matter of urgency.

Published

2023

2. Loss-of-function mutations in ADCY3cause monogenic severe obesity

Author

Saeed, Sadia, Bonnefond, Amélie, Tamanini, Filippo, Mirza, Muhammad Usman, Manzoor, Jaida, Janjua, Qasim M., Din, Sadia M., Gaitan, Julien, Milochau, Alexandra, Durand, Emmanuelle, Vaillant, Emmanuel, Haseeb, Attiya, De Graeve, Franck, Rabearivelo, Iandry, Sand, Olivier, Queniat, Gurvan, Boutry, Raphaël, Schott, Dina A., Ayesha, Hina, Ali, Muhammad, Khan, Waqas I., Butt, Taeed A., Rinne, Tuula, Stumpel, Connie, Abderrahmani, Amar, Lang, Jochen, Arslan, Muhammad, and Froguel, Philippe

Abstract

Study of monogenic forms of obesity has demonstrated the pivotal role of the central leptin–melanocortin pathway in controlling energy balance, appetite and body weight1. The majority of loss-of-function mutations (mostly recessive or co-dominant) have been identified in genes that are directly involved in leptin–melanocortin signaling. These genes, however, only explain obesity in <5% of cases, predominantly from outbred populations2. We previously showed that, in a consanguineous population in Pakistan, recessive mutations in known obesity-related genes explain ~30% of cases with severe obesity3–5. These data suggested that new monogenic forms of obesity could also be identified in this population. Here we identify and functionally characterize homozygous mutations in the ADCY3gene encoding adenylate cyclase 3 in children with severe obesity from consanguineous Pakistani families, as well as compound heterozygous mutations in a severely obese child of European-American descent. These findings highlight ADCY3 as an important mediator of energy homeostasis and an attractive pharmacological target in the treatment of obesity.

Published

2018