The FAM13A Long Isoform Regulates Cilia Movement and Coordination in Airway Mucociliary Transport

Ashleigh Howes; Clare Rogerson; Nikolai Belyaev; Tina Karagyozova; Radu Rapiteanu; Ricardo Fradique; Nicola Pellicciotta; David Mayhew; Catherine Hurd; Stefania Crotta; Tanya Singh; Kevin Dingwell; Anniek Myatt; Navot Arad; Hikmatyar Hasan; Hielke Bijlsma; Aliza Panjwani; Vinaya Vijayan; George Young; Angela Bridges; Sebastien Petit-Frere; Joanna Betts; Chris Larminie; James C Smith; Edith M Hessel; David Michalovich; Louise Walport; Pietro Cicuta; Andrew J Powell; Soren Beinke; Andreas Wack

doi:10.1165/rcmb.2024-0063OC

The FAM13A Long Isoform Regulates Cilia Movement and Coordination in Airway Mucociliary Transport

Am J Respir Cell Mol Biol. 2024 Sep;71(3):282-293. doi: 10.1165/rcmb.2024-0063OC.

Authors

Ashleigh Howes^{1

2}, Clare Rogerson^{1

3}, Nikolai Belyaev², Tina Karagyozova⁴, Radu Rapiteanu⁴, Ricardo Fradique⁵, Nicola Pellicciotta⁵, David Mayhew⁶, Catherine Hurd^{7

3}, Stefania Crotta¹, Tanya Singh⁶, Kevin Dingwell⁸, Anniek Myatt⁹, Navot Arad⁹, Hikmatyar Hasan⁹, Hielke Bijlsma⁹, Aliza Panjwani², Vinaya Vijayan¹⁰, George Young¹¹, Angela Bridges¹², Sebastien Petit-Frere², Joanna Betts⁶, Chris Larminie⁶, James C Smith⁸, Edith M Hessel¹³, David Michalovich², Louise Walport⁷, Pietro Cicuta⁵, Andrew J Powell³, Soren Beinke², Andreas Wack¹

Affiliations

¹ Immunoregulation Laboratory.
² Immunology Research Unit.
³ Crick-GSK Biomedical LinkLabs.
⁴ Functional Genomics.
⁵ Cavendish Laboratory, University of Cambridge, Cambridge, United Kingdom.
⁶ Computational Biology, and.
⁷ Protein-Protein Interaction Laboratory.
⁸ Developmental Biology Laboratory, and.
⁹ Capgemini Engineering, Capgemini UK, Stevenage, United Kingdom; and.
¹⁰ Development Digital and Tech, GSK, Collegeville, Pennsylvania.
¹¹ Bioinformatics and Biostatistics, The Francis Crick Institute, London, United Kingdom.
¹² Protein, Cellular and Structural Sciences.
¹³ Refractory Respiratory Inflammation Discovery Performance Unit, GSK R&D, Stevenage, United Kingdom.

Abstract

Single nucelotide polymorphisms (SNPs) at the FAM13A locus are among the most commonly reported risk alleles associated with chronic obstructive pulmonary disease (COPD) and other respiratory diseases; however, the physiological role of FAM13A is unclear. In humans, two major protein isoforms are expressed at the FAM13A locus: "long" and "short," but their functions remain unknown, partly because of a lack of isoform conservation in mice. We performed in-depth characterization of organotypic primary human airway epithelial cell subsets and show that multiciliated cells predominantly express the FAM13A long isoform containing a putative N-terminal Rho GTPase-activating protein (RhoGAP) domain. Using purified proteins, we directly demonstrate the RhoGAP activity of this domain. In Xenopus laevis, which conserve the long-isoform, Fam13a deficiency impaired cilia-dependent embryo motility. In human primary epithelial cells, long-isoform deficiency did not affect multiciliogenesis but reduced cilia coordination in mucociliary transport assays. This is the first demonstration that FAM13A isoforms are differentially expressed within the airway epithelium, with implications for the assessment and interpretation of SNP effects on FAM13A expression levels. We also show that the long FAM13A isoform coordinates cilia-driven movement, suggesting that FAM13A risk alleles may affect susceptibility to respiratory diseases through deficiencies in mucociliary clearance.

Keywords: COPD; airways; cilia movement; mucociliary clearance; multiciliated cells.

MeSH terms

Animals
Cells, Cultured
Cilia* / metabolism
Epithelial Cells / metabolism
GTPase-Activating Proteins* / genetics
GTPase-Activating Proteins* / metabolism
Humans
Mucociliary Clearance*
Protein Isoforms* / genetics
Protein Isoforms* / metabolism
Respiratory Mucosa / metabolism
Xenopus Proteins / genetics
Xenopus Proteins / metabolism
Xenopus laevis*

Substances

FAM13A protein, human
GTPase-Activating Proteins
Protein Isoforms
Xenopus Proteins

Abstract

MeSH terms

Substances

Grants and funding