AI Article Synopsis

  • Meckel syndrome, nephronophthisis, Joubert syndrome, and Bardet-Biedl syndrome are linked to mutations in proteins at the ciliary transition zone, indicating these proteins may have different functions but can also lead to multiple syndromes from mutations in a single gene.
  • A study analyzed ten zebrafish mutants for these TZ proteins, revealing variation in phenotypes that suggest specific tissue functions and highlighting that different outcomes can occur from mutations in the same gene.
  • The research also showed that unique CRISPR/Cas9 techniques can replicate certain genetic phenotypes and has identified several new gene candidates associated with ciliary functions.

Article Abstract

Meckel syndrome, nephronophthisis, Joubert syndrome and Bardet-Biedl syndrome are caused by mutations in proteins that localize to the ciliary transition zone (TZ). The phenotypically distinct syndromes suggest that these TZ proteins have differing functions. However, mutations in a single TZ gene can result in multiple syndromes, suggesting that the phenotype is influenced by modifier genes. We performed a comprehensive analysis of ten zebrafish TZ mutants, including mks1, tmem216, tmem67, rpgrip1l, cc2d2a, b9d2, cep290, tctn1, nphp1 and nphp4, as well as mutants in ift88 and ift172. Our data indicate that variations in phenotypes exist between different TZ mutants, supporting different tissue-specific functions of these TZ genes. Further, we observed phenotypic variations within progeny of a single TZ mutant, reminiscent of multiple disease syndromes being associated with mutations in one gene. In some mutants, the dynamics of the phenotype became complex with transitory phenotypes that are corrected over time. We also demonstrated that multiple-guide-derived CRISPR/Cas9 F0 'crispant' embryos recapitulate zygotic null phenotypes, and rapidly identified ciliary phenotypes in 11 cilia-associated gene candidates (ankfn1, ccdc65, cfap57, fhad1, nme7, pacrg, saxo2, c1orf194, ttc26, zmynd12 and cfap52).

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9844136PMC
http://dx.doi.org/10.1242/dmm.049568DOI Listing

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