Gain-of-function variants in SMAD4 compromise respiratory epithelial function

• Published in: Journal of allergy and clinical immunology Vol. 155; no. 1; pp. 107 - 119.e2
• Main Authors: Lindsay, Mark E., Scimone, Eleanor R., Lawton, Joseph, Richa, Rashmi, Yonker, Lael M., Di, Yuanpu P., Buch, Karen, Ouyang, Wukun, Mo, Xiulei, Lin, Angela E., Mou, Hongmei
• Format: Journal Article
• Language: English
• Published: United States Elsevier Inc 01.01.2025
• Subjects: cell proliferation; innate immunity; mucociliary differentiation; Myhre syndrome; nasal epithelial basal cells; SMAD4 mutation; mucociliary differentiation; SMAD4; cell proliferation; BMP; PPI; GST; SPLUNC1; SMAD4 mutation; Myhre syndrome; VF; innate immunity; PAO1; nasal epithelial basal cells; WT; ALI; TR-FRET; GOF
• ISSN: 0091-6749; 1097-6825; 1097-6825
• DOI: 10.1016/j.jaci.2024.08.024

[Display omitted] Myhre syndrome is an exceedingly rare yet increasingly diagnosed genetic disorder arising from germline variants in the SMAD4 gene. Its core manifestation is the progression of stiffness and fibrosis across multiple organs. Individuals with Myhre syndrome exhibit a propensity for upper respiratory tract remodeling and infections. The molecular and cellular mechanisms underlying this phenotype remain unclear. We sought to investigate how SMAD4 pathogenic variants associated with Myhre syndrome affect SMAD4 protein levels, activation, and physiological functions in patient-derived nasal epithelial cells. Clinical observations were conducted on a cohort of 47 patients recruited at Massachusetts General Hospital from 2016 to 2023. Nasal epithelial basal cells were isolated and cultured from inferior turbinate brushings of healthy subjects (n = 8) and patients with Myhre syndrome (n = 3; SMAD4-Ile500Val, Arg496Cys, and Ile500Thr). Transcriptomic analysis and functional assays were performed to assess SMAD4 levels, transcriptional activity, and epithelial cell host defense functions, including cell proliferation, mucociliary differentiation, and bacterial elimination. Clinical observations revealed a prevalent history of otitis media and sinusitis among most individuals with Myhre syndrome. Analyses of nasal epithelial cells indicated that SMAD4 mutations do not alter SMAD4 protein stability or upstream regulatory SMAD phosphorylation but enhance signaling transcriptional activity, supporting a gain-of-function mechanism, likely attributable to increased protein-protein interaction of the SMAD complex. Consequently, Myhre syndrome nasal basal cells exhibit reduced potential in cell proliferation and mucociliary differentiation. Furthermore, Myhre syndrome nasal epithelia are impaired in bacterial killing. Compromised innate immunity originating from epithelial cells in Myhre syndrome may contribute to increased susceptibility to upper respiratory tract infections.