Certain heterozygous variants in the kinase domain of the serine/threonine kinase NEK8 can cause an autosomal dominant form of polycystic kidney disease

Claus, Laura; Chen, Chuan; Stallworth, Jennifer L.; Turner, Joshua L.; Slaats, Gisela G.; Hawks, Alexandra L.; Mabillard, Holly; Senum, Sarah R.; Srikanth, Sujata; Flanagan-Steet, Heather; Louie, Raymond J.; Silver, Josh; Lerner‐Ellis, Jordan; Morel, Chantal F.; Mighton, Chloe; Sleutels, Frank; Slegtenhorst, Marjon van; Ham, Tjakko J. van; Brooks, Alice S.; Dorresteijn, Eiske M.; Barakat, Tahsin Stefan; Dahan, Karin; Demoulin, Nathalie; Goffin, Éric; Olinger, Eric; Larsen, Martin Jakob; Hertz, Jens Michael; Lilien, Marc R.; Obeidová, Lena; Seeman, Tomáš; Stone, Hillarey K.; Kerecuk, Larissa; Gurgu, M.; Yengej, Fjodor A. Yousef; Ammerlaan, Carola; Rookmaaker, Maarten B.; Hanna, Christian; Rogers, R. Curtis; Duran, Karen; Peters, E. D. J.; Sayer, John A.; Haaften, Gijs van; Harris, Peter C.; Ling, Kun; Mason, Jennifer M.; Eerde, Albertien M. van; Steet, Richard; Ambrose, J. C.; Arumugam, Prabhu; Bevers, R.; Bleda, Marta; Boardman-Pretty, F.; Boustred, C. R.; Brittain, Helen; Caulfield, Mark J.; Chan, G. C.; Elgar, Greg; Fowler, Tom; Giess, Adam; Hamblin, Angela; Henderson, Shirley; Hubbard, Tim; Jackson, Robert B.; Jones, Louise; Kasperavičiūtė, Dalia; Kayikci, Melis; Kousathanas, Athanasios; Lahnstein, L.; Leigh, Sarah; Leong, I. U. S.; López, Javier Ferreiros; Maleady‐Crowe, F.; McEntagart, Meriel; Minneci, Federico; Moutsianas, Loukas; Mueller, Michael; Murugaesu, Nirupa; Need, Anna C.; O’Donovan, Peter; Odhams, C. A.; Patch, Christine; Pereira, Mariana Buongermino; Perez-Gil, D.; Pullinger, J.; Rahim, T.; Rendon, Augusto; Rogers, Tim; Savage, K.; Sawant, K.; Scott, Richard; Siddiq, Afshan; Sieghart, A.; Smith, Samuel C.; Sosinsky, Alona; Stuckey, Alexander; Tanguy, M.; Tavares, Ana Lisa Taylor; Thomas, Ellen; Thompson, S. R.; Tucci, Arianna; Welland, M. J.; Williams, Eleanor; Witkowska, K.; Wood, S. M.

doi:10.1016/j.kint.2023.07.021

Cited by 5 publications

(3 citation statements)

References 45 publications

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“…ANKS6 transports NEK8 from the cytoplasm to the cilia, where it is phosphorylated in the presence of INV and NPHP3, suggesting its role as both a substrate and a functional activator of NEK8 kinase activity [59]. NEK8 has already been identified as an important regulator in kidney and liver cystogenesis and seems to be involved in the same signaling cascade as PKD1 and PKD2 [60,61]. Moreover, a study by Nakajima et al has demonstrated that the IC functions as an intraciliary signal-generating center and that ANKS6 may be involved in the transmission of signals from cilia to the cytoplasm [62], possibly indicating that the phosphorylation status of ANKS6 influences the stability of the protein [47,62,63].…”

Section: Role Of Samcystin In Cystogenesismentioning

confidence: 99%

The Han:SPRD Rat: A Preclinical Model of Polycystic Kidney Disease

Kofotolios,

Bonios,

Adamopoulos

et al. 2024

Biomedicines

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Autosomal Dominant Polycystic Kidney Disease (ADPKD) stands as the most prevalent hereditary renal disorder in humans, ultimately culminating in end-stage kidney disease. Animal models carrying mutations associated with polycystic kidney disease have played an important role in the advancement of ADPKD research. The Han:SPRD rat model, carrying an R823W mutation in the Anks6 gene, is characterized by cyst formation and kidney enlargement. The mutated protein, named Samcystin, is localized in cilia of tubular epithelial cells and seems to be involved in cystogenesis. The homozygous Anks6 mutation leads to end-stage renal disease and death, making it a critical factor in kidney development and function. This review explores the utility of the Han:SPRD rat model, highlighting its phenotypic similarity to human ADPKD. Specifically, we discuss its role in preclinical trials and its importance for investigating the pathogenesis of the disease and developing new therapeutic approaches.

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Section: Role Of Samcystin In Cystogenesismentioning

confidence: 99%

The Han:SPRD Rat: A Preclinical Model of Polycystic Kidney Disease

Kofotolios,

Bonios,

Adamopoulos

et al. 2024

Biomedicines

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“…This has nevertheless been observed in some nephropathies, like the IFT140 , NEK8 , or NPHS2 -associated ones. While their biallelic loss-of-function variants cause Mainzer-Saldino syndrome [ 16 ], renal-hepatic-pancreatic dysplasia [ 17 – 19 ], or steroid-resistant nephrotic syndrome [ 20 ], respectively, monoallelic variants of IFT140 and NEK8 were found causal in rare forms of ADPKD [ 21 – 23 ] and those of NPHS2 in focal segmental glomerulosclerosis (FSGS) [ 24 ]. The monoallelic variants were specific in NEK8 (i.e., p.R45W) [ 21 , 22 ] and in NPHS2 (p.L330Vfs*15 with a premature stop in the last exon) [ 24 ], suggesting a dominant negative effect [ 21 ], but the IFT140 variants in mild ADPKD are intriguingly loss-of-function variants [ 23 ].…”

Section: The Changing Face Of Dominancementioning

confidence: 99%

“…While their biallelic loss-of-function variants cause Mainzer-Saldino syndrome [ 16 ], renal-hepatic-pancreatic dysplasia [ 17 – 19 ], or steroid-resistant nephrotic syndrome [ 20 ], respectively, monoallelic variants of IFT140 and NEK8 were found causal in rare forms of ADPKD [ 21 – 23 ] and those of NPHS2 in focal segmental glomerulosclerosis (FSGS) [ 24 ]. The monoallelic variants were specific in NEK8 (i.e., p.R45W) [ 21 , 22 ] and in NPHS2 (p.L330Vfs*15 with a premature stop in the last exon) [ 24 ], suggesting a dominant negative effect [ 21 ], but the IFT140 variants in mild ADPKD are intriguingly loss-of-function variants [ 23 ]. Such transformations of dominant or recessive phenotypes would have reversed the two forms of a trait in Mendel’s experiment, but would not have changed the 3:1 ratio of the dominant and recessive forms in the second generation.…”

Section: The Changing Face Of Dominancementioning

confidence: 99%

The dominant findings of a recessive man: from Mendel’s kid pea to kidney

Tory

2023

Pediatr Nephrol

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The research of Mendel, born two centuries ago, still has many direct implications for our everyday clinical work. He introduced the terms “dominant” and “recessive” characters and determined their 3:1 ratio in the offspring of heterozygous “hybrid” plants. This distribution allowed calculation of the number of the phenotype-determining “elements,” i.e., the alleles, and has been used ever since to prove the monogenic origin of a disorder. The Mendelian inheritance of monogenic kidney disorders is still of great help in distinguishing them from those with multifactorial origin in clinical practice. Inheritance of most monogenic kidney disorders fits to Mendel’s observations: the equal contribution of the two parents and the complete penetrance or the direct correlation between the frequency of the recessive character and the degree of inbreeding. Nevertheless, beyond the truth of these basic concepts, several observations have expanded their genetic characteristics. The extreme genetic heterogeneity, the pleiotropy of the causal genes and the role of modifiers in ciliopathies, the digenic inheritance and parental imprinting in some tubulopathies, and the incomplete penetrance and eventual interallelic interactions in podocytopathies, reflect this expansion. For all these reasons, the transmission pattern in a natural setting may depend not only on the “character” but also on the causal gene and the variant. Mendel’s passion for research combined with his modest personality and meticulous approach can still serve as an example in the work required to understand the non-Mendelian universe of genetics.

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