Characterization of the Cystic Phenotype Associated with Monoallelic ALG8 and ALG9 Pathogenic Variants

Tabinda Jawaid; Doaa E Elbarougy; Sravanthi Lavu; Guillaume Buia; Sarah R Senum; Eric Olinger; Hana Yang; Shannon K McDonnell; Joshua T Bublitz; Jun Ma; Marie-Pierre Audrézet; Charles D Madsen; Rachel S Schauer; Tracy A Baker; Adriana V Gregory; Sarah E Orr; Miguel Barroso-Gil; Ruxandra Neatu; Giancarlo Joli; Neera K Dahl; Timothy L Kline; Valentine Gillion; Karin Dahan; Francois Jouret; Ronald D Perrone; Theodore I Steinman; Dorien J M Peters; Berenice Y Gitomer; Terry J Watnick; Eliecer Coto; Fouad T Chebib; Marie C Hogan; Janet E Olson; Nicholas B Larson; Elisabet Ars; Jan Halbritter; Nathalie Demoulin; Vicente E Torres; John A Sayer; Emilie Cornec-Le Gall; Peter C Harris; Genomics England Research Consortium, UK Biobank, HALT PKD, DIPAK, TAME PKD, Genkyst studies, Mayo Clinic Biobank, and Regeneron Genetics Center

doi:10.1681/ASN.0000000613

Characterization of the Cystic Phenotype Associated with Monoallelic ALG8 and ALG9 Pathogenic Variants

J Am Soc Nephrol. 2025 Jun 1;36(6):1056-1071. doi: 10.1681/ASN.0000000613. Epub 2025 Feb 3.

Authors

Tabinda Jawaid¹, Doaa E Elbarougy¹, Sravanthi Lavu¹, Guillaume Buia^{2

3}, Sarah R Senum¹, Eric Olinger^{4

5}, Hana Yang¹, Shannon K McDonnell⁶, Joshua T Bublitz⁶, Jun Ma⁷, Marie-Pierre Audrézet^{2

3}, Charles D Madsen¹, Rachel S Schauer¹, Tracy A Baker¹, Adriana V Gregory¹, Sarah E Orr⁴, Miguel Barroso-Gil⁴, Ruxandra Neatu⁴, Giancarlo Joli^{1

8}, Neera K Dahl¹, Timothy L Kline⁹, Valentine Gillion^{10

11

12}, Karin Dahan^{12

13}, Francois Jouret¹⁴, Ronald D Perrone¹⁵, Theodore I Steinman¹⁶, Dorien J M Peters¹⁷, Berenice Y Gitomer¹⁸, Terry J Watnick¹⁹, Eliecer Coto²⁰, Fouad T Chebib²¹, Marie C Hogan¹, Janet E Olson²², Nicholas B Larson⁶, Elisabet Ars²³, Jan Halbritter^{24

25}, Nathalie Demoulin^{10

11

12}, Vicente E Torres¹, John A Sayer^{4

26}, Emilie Cornec-Le Gall^{2

3}, Peter C Harris^{1

27}; Genomics England Research Consortium, UK Biobank, HALT PKD, DIPAK, TAME PKD, Genkyst studies, Mayo Clinic Biobank, and Regeneron Genetics Center

Collaborators

Genomics England Research Consortium, UK Biobank, HALT PKD, DIPAK, TAME PKD, Genkyst studies, Mayo Clinic Biobank, and Regeneron Genetics Center:
John C Ambrose, Prabhu Arumugam, Roel Bevers, Marta Bleda, Freya Boardman-Pretty, Christopher R Boustred, Helen Brittain, Mark J Caulfield, Georgia C Chan, Greg Elgar, Tom Fowler, Adam Giess, Angela Hamblin, Shirley Henderson, Tim J P Hubbard, Rob Jackson, Louise J Jones, Dalia Kasperaviciute, Melis Kayikci, Athanasios Kousathanas, Lea Lahnstein, Sarah E A Leigh, Ivonne U S Leong, Javier F Lopez, Fiona Maleady-Crowe, Meriel McEntagart, Federico Minneci, Loukas Moutsianas, Michael Mueller, Nirupa Murugaesu, Anna C Need, Peter O'Donovan, Chris A Odhams, Christine Patch, Mariana Buongermino Pereira, Daniel Perez-Gil, John Pullinger, Tahrima Rahim, Augusto Rendon, Tim Rogers, Kevin Savage, Kushmita Sawant, Richard H Scott, Afshan Siddiq, Alexander Sieghart, Samuel C Smith, Alona Sosinsky, Alexander Stuckey, Mélanie Tanguy, Ana Lisa Taylor Tavares, Ellen R A Thomas, Simon R Thompson, Arianna Tucci, Matthew J Welland, Eleanor Williams, Katarzyna Witkowska, Suzanne M Wood, A B Chapman, A Yu, F T Winklhofer, M Mrug, K T Bae, K Z Abebe, C G Patterson, G M Brosnahan, W E Braun, F F Rahbari Oskoui, P G Czarnecki, D Miskulin, D P Landsittel, W M Bennett, Corinne Antignac, Bouthéina Ben Taarit, Béatrice Birmele, Olivia Boyer, Deborah Talmud, Aurélie Hummel, Marie Haeck, Marianne Hupe, Bertrand Knebelmann, Aurélie Lavergne, Béatrice Laudier, Camille Lanaret, Alice Le Clech, Jean-David Zeitoun, Caroline Preissig, Emmanuel Esteve, Sophie Chauvet, Ott Julien, Eric Michez, Mathilde Tamain, Myriam Dao, Nicolas Peters, Camille Saint Jacques, Sylvie Odent, Leila Chenine, Marion Gerbal, Deborah Talmud, Y Le Meur, A Grall, M C Moal, T Tanquerel, C Hanrotel, I Segalen, L Lanfranco, C Mesguen, A Kersale, A Capdeville, V Huynh, M Hourmant, J Dantal, M Giral, A Meurette, M Lino, C Garandeau, B Hodemon-Corne, E Allain-Launay, D Cantarovich, G Blancho, D Hristea, G Couvrat, F Fakhouri, F Lavainne, C Vercel, M Chapal, A Le Fur, C Gourrau, C Deltombe C, C Vigneau, M P Morin, P Le Pogamp, T Frouget, S Gie, J Rivalan, E Laruelle, C Richer, N Lorcy, L Golbin, M Terrasse, S Morice, H Brenier, A Michel, E Tomkiewicz, Q L Nguyen, E Vabret, A Lavergne, E Pierre, J Chemouny, J M Halimi, H Longuet, P Gatault, E Merieau, C Barbet, M Buchler, G Golea, L Ghouti, D Gautard, B Sautenet, M François, A Fournier, C Baron, C Salmon, N Rabot, L Prat, J F Valentin, E Chevallier, B Birmele, C Genest, N Goin, A Goumard, F Bridoux, E Desport, A Thierry, L Ecotiere, G Touchard, M Belmouaz, V Javaugue, M Bauwens, F Fride-Leroy, G Goussard, I Bouteau, L Jacquemont, J F Subra, J F Augusto, A Duveau, V Besson, M Cousin, J Sayegh, C Onno, M N Maghakian, J Demiselle, C Deschamps, A S Garnier, F Guibert, M Planchais, C Charasse, C Stanescu, P Le Cacheux, S Baluta, F Leonetti, R Boulahrouz, M L Ferrier, C Freguin, A Simon, J Potier, J M Coulibaly, A Delezire, E Renaudineau, T Dolley-Hitze, R Perrichot, E Michez, L Mandart, V Menoyo, E Pincon, C Muresan, P Y Durand, L Corlu, I Wegner, P Siohan, I Metes, T Guyon-Roger, B Wehbe, L Gueguen, C Drouet, C Loheac, T Sawadogo, A Le Guillou, M Le Jeune, G Beillard, S Lefevre, C Chamontin, S Georgescu, P Jousset, R Latif, M Massad, J P Jaulin, G Couvrat, A H Querard, J N Ottavioli, N Target, A Chapal, A Le Fur, V Charpy, D Besnier, S Regnier-Le Coz, A Blanpain, S Durault, D Larmet, A Le Clech, L M Pouteau, D Labatut, J P Coindre, M Sigogne, G Piccoli, C Bachelet-Rousseau, S Delbes, O Fritz, B Pourreau, S Mzoughi, M P Guillodo, M Gosselin, P Depraetre, B Strullu, E Chaffara, M Le Mee, N Terki, K Goulesque, S Benarbia, M Dimulescu, M Rifaat, G Duneau, D Legrand, E Georges, G Seret, F Babinet, S Lanoiselee, C Savoiu, A Testa, I Oancea, I Coupel, S Parahy, G Lefrancois, E Briand, D Bugnon, F W Visser, N F Casteleijn, M D A van Gastel, A L Messchendorp, M K Neijenhuis, M J Pena, E M Spithoven, H M A D'Agnolo, M A Lantinga, T J Gevers, J F Wetzels, J P H Drenth, M Salih, R Zietse, D Soonawala, J W de Fijter, Goncalo Abecasis, Aris Baras, Michael Cantor, Giovanni Coppola, Andrew Deubler, Aris Economides, Luca A Lotta, John D Overton, Jeffrey G Reid, Katherine Siminovitch, Alan Shuldiner, Christina Beechert, CaitlinForsythe, Erin D Fuller, Zhenhua Gu, Michael Lattari, Alexander Lopez, John D Overton, Maria Sotiropoulos Padilla, Manasi Pradhan, Kia Manoochehri, Thomas D Schleicher, Louis Widom, Sarah E Wolf, Ricardo H Ulloa, Amelia Averitt, Nilanjana Banerjee, Michael Cantor, Dadong Li, Sameer Malhotra, Ob Deepika Sharma, Jeffrey Staples, Xiaodong Bai, Suganthi Balasubramanian, Suying Bao, Boris Boutkov, Siying Chen, Gisu Eom, Lukas Habegger, Alicia Hawes, Shareef Khalid, Olga Krasheninina, Rouel Lanche, Adam J Mansfield, Evan K Maxwell, George Mitra, Mona Nafde, Sean O'Keeffe, Max Orelus, Razvan Panea, Tommy Polanco, Ayesha Rasool, Jeffrey G Reid, William Salerno, Jeffrey C Staples, Kathie Sun, Goncalo Abecasis, Joshua Backman, AmyDamask, Lee Dobbyn, Manuel Allen Revez Ferreira, Arkopravo Ghosh, Christopher Gillies, Lauren Gurski, Eric Jorgenson, Hyun Min Kang, Michael Kessler, Jack Kosmicki, Alexander Li, Nan Lin, Daren Liu, Adam Locke, Jonathan Marchini, Anthony Marcketta, Joelle Mbatchou, Arden Moscati, Charles Paulding, Carlo Sidore, Eli Stahl, Kyoko Watanabe, Bin Ye, Blair Zhang, Andrey Ziyatdinov, Ariane Ayer, Aysegul Guvenek, George Hindy, Giovanni Coppola, Jan Freudenberg, Jonas Bovijn, Katherine Siminovitch, Kavita Praveen, Luca A Lotta, Manav Kapoor, Mary Haas, Moeen Riaz, Niek Verweij, Olukayode Sosina, Parsa Akbari, Priyanka Nakka, Sahar Gelfman, Sujit Gokhale, Tanima De, Veera Rajagopal, Alan Shuldiner, Bin Ye, Gannie Tzoneva, Juan Rodriguez-Flores, Esteban Chen, Marcus B Jones, Michelle G LeBlanc, Jason Mighty, Lyndon J Mitnaul, Nirupama Nishtala, Nadia Rana, Jaimee Hernandez

Affiliations

¹ Division of Nephrology and Hypertension, Mayo Clinic, Rochester, Minnesota.
² Inserm, UMR 1078, GGB, CHU Brest, University of Brest, Brest, France.
³ Centre de Références Maladies Rénales Hérédiatires de l'Enfant et de l'Adulte MARHEA, Filière ORKID, CHU, Brest, France.
⁴ Faculty of Medical Sciences, Translational and Clinical Research Institute, Newcastle University, Newcastle upon Tyne, United Kingdom.
⁵ Center for Human Genetics, Cliniques Universitaires Saint-Luc, Brussels, Belgium.
⁶ Department of Quantitative Health Sciences, Mayo Clinic, Rochester, Minnesota.
⁷ Division of Computational Biology, Mayo Clinic, Rochester, Minnesota.
⁸ IRCCS San Raffaele Scientific Institute, University Vita Salute San Raffaele, Milan, Italy.
⁹ Department of Radiology, Mayo Clinic, Rochester, Minnesota.
¹⁰ Division of Nephrology, Cliniques Universitaires Saint-Luc, UCLouvain, Brussels, Belgium.
¹¹ Recherche Expérimentale et Clinique, UCLouvain, Brussels, Belgium.
¹² European Reference Network for Rare Kidney Diseases (ERKNet), Center of Human Genetics, Charleroi, Belgium.
¹³ Institute Pathology and Genetic, Center of Human Genetics, Charleroi, Belgium.
¹⁴ Division of Nephrology, University of Liège, Liège, Belgium.
¹⁵ Division of Nephrology, Tufts Medical Center and Tufts University School of Medicine, Boston, Massachusetts.
¹⁶ Renal Division, Beth Israel Deaconess Medical Center, Boston, Massachusetts.
¹⁷ Department of Human Genetics, Leiden University Medical Center, Leiden, The Netherlands.
¹⁸ Division of Renal Diseases and Hypertension, University of Colorado School of Medicine, University of Colorado Anschutz Medical Campus, Aurora, Colorado.
¹⁹ Division of Nephrology, University of Maryland School of Medicine, Baltimore, Maryland.
²⁰ Department of Medicine and RICORS-2040 (Kidney Disease), University of Oviedo, Oviedo, Spain.
²¹ Division of Nephrology and Hypertension, Mayo Clinic, Jacksonville, Florida.
²² Division of Epidemiology, Mayo Clinic, Rochester, Minnesota.
²³ Molecular Biology Laboratory, Fundació Puigvert, Instituto de Investigaciones Biomédicas Sant Pau (IIB-Sant Pau), RICORS2040 (Kidney Disease), Universitat Autònoma de Barcelona, Barcelona, Spain.
²⁴ Department of Nephrology, Charité - Universitätsmedizin Berlin, Freie Universität Berlin and Humboldt-Universität zu Berlin, Berlin, Germany.
²⁵ Division of Nephrology, Department of Internal Medicine, University of Leipzig Medical Center, Leipzig, Germany.
²⁶ Renal Services, Newcastle Upon Tyne Hospitals NHS Foundation Trust, and NIHR Newcastle Biomedical Research Centre, Newcastle University, Newcastle upon Tyne, United Kingdom.
²⁷ Department of Biochemistry and Molecular Biology, Mayo Clinic, Rochester, Minnesota.

PMID: 39899384
PMCID: PMC12147961 (available on 2026-06-01)
DOI: 10.1681/ASN.0000000613

Abstract

Key Points:

Loss-of-function ALG8 and ALG9 variants were enriched in polycystic kidney/liver groups and International Classification of Diseases–coded cystic individuals in population cohorts.
The ALG8 and ALG9 kidney phenotypes were usually mild to moderate, and lower eGFR or kidney failure was rare.
ALG8 pathogenic variants sometimes resulted in severe polycystic liver disease.

Background: Autosomal dominant polycystic kidney disease (ADPKD) is a common, inherited nephropathy often resulting in kidney failure. It is genetically heterogeneous; along with the major genes, PKD1 and PKD2, at least eight others have been suggested. ALG8 pathogenic variants have been associated with autosomal dominant polycystic liver disease and implicated in ADPKD, while ALG9 has been suggested as an ADPKD gene, but details of the phenotypes and penetrance are unclear.

Methods: We screened >3900 families with cystic kidneys and/or livers using global approaches to detect ALG8 or ALG9 pathogenic variants. In addition, population cohorts with sequence data (Genomics England 100K Genomics Project, UK Biobank, and Mayo Clinic Biobank [MCBB]) were screened for ALG8/ALG9 pathogenic variants.

Results: Multicenter screening of individuals with polycystic kidney and/or liver disease identified 51 (1.3%) ALG8 (7 multiplex) and 23 (0.6%) ALG9 (5 multiplex) families—frequencies that were approximately 10× and approximately 24× greater than nonpolycystic kidney disease controls. Analysis of individuals with polycystic kidney disease phenotypes in 100K Genomics Project, UK Biobank, and MCBB identified nine ALG8 (0.39%) and nine ALG9 (0.39%) families, an enriched frequency over controls. Two individuals had PKD1 and ALG8 pathogenic changes. Eighty-nine percent of individuals with ALG8 mutations with imaging in the entire MCBB had kidney cysts (50%, >10 cysts), with greater median kidney and liver cyst numbers than controls. For ALG9, 78% had kidney cysts (27%, >10 cysts). Individuals with ALG8 mutations typically had mild cystic kidneys with limited enlargement. Liver cysts were common (71%), with enlarged livers (>2L) found in 11 of 62 patients, although surgical intervention was rare. The ALG9 kidney phenotype was also of mild cystic kidneys, but enlarged livers were rare; for both genes, CKD or kidney failure were rare.

Conclusions: ALG8 and ALG9 are defined as cystic kidney/liver genes but with limited penetrance for lower eGFR.

Keywords: ADPKD; genetic diseases and development; nephropathy; polycystic kidney disease.

Abstract

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