Twenty-three (88.5%) of the 26 BS patients involved in this study had CLCNKB mutations. The p.W610X mutation and large deletion were two common types of mutations in CLCNKB. The clinical manifestations of BS III were heterogeneous without a genotype-phenotype correlation, typically manifesting cBS phenotype but also aBS or mixed Bartter-Gitelman phenotypes. The molecular diagnostic steps for patients with BS in our population should be designed taking these peculiar genotype distributions into consideration, and a new more clinically relevant classification including BS and Gitelman syndrome is required.
Eujin Park, Chung Lee, Nayoung Kim, Yo Han Ahn, Young Ho Park, Joo Hoon Lee, Seong Heon Kim, Min Cho, Heeyeon Cho, Kee Yoo, Jae Il Shin, Hee Gyung Kang, Il Soo Ha, Woong‐Yang Park, Hae Il Cheong
Jessica Caprioli, Paola Bettinaglio, Peter F. Zipfel, Barbara Amadei, Erica Daina, Sara Gamba, Christine Skerka, Nicola Marziliano, Giuseppe Remuzzi, Marina Noris
Elena Bresin, Erica Rurali, Jessica Caprioli, Pilar Sánchez‐Corral, Véronique Frémeaux‐Bacchi, Santiago Rodrı́guez de Córdoba, Sheila Pinto, Timothy H.J. Goodship, Marta Alberti, David Ribes, Elisabetta Valoti, Giuseppe Remuzzi, Marina Noris
Rubén Martínez-Barricarte, Gaia Pianetti, Ruxandra Gautard, Joachim Misselwitz, Lisa Strain, Véronique Frémeaux‐Bacchi, Christine Skerka, Peter F. Zipfel, Tim Goodship, Marina Noris, Giuseppe Remuzzi, Santiago Rodrı́guez de Córdoba
Catherine Couture, Alexandru Saveanu, Anne Barlier, Jean‐Claude Carel, Martin Faßnacht, C.E. Flück, Muriel Houang, Michael Maes, Franziska Phan-Hug, A Enjalbert, Jacques Drouin, Thierry Brue, Sophie Vallette
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