Abstract
The murine beige mutant phenotype and the human Chediak-Higashi syndrome are caused by mutations in the murine Lyst (lysosomal trafficking regulator) gene and the human CHS gene, respectively. In this report we have analyzed a novel murine mutant Lyst allele, called Lystbg-grey, that had been found in an ENU mutation screen and named grey because of the grey coat color of affected mice. The phenotype caused by the Lystbg-grey mutation was inherited in a recessive fashion. Melanosomes of melanocytes associated with hair follicles and the choroid layer of the eye, as well as melanosomes in the neural tube-derived pigment epithelium of the retina, were larger and irregularly shaped in homozygous mutants compared with those of wild-type controls. Secretory vesicles in dermal mast cells of the mutant skin were enlarged as well. Test crosses with beige homozygous mutant mice (Lystbg) showed that double heterozygotes (Lystbg/Lystbg-grey) were phenotypically indistinguishable from either homozygous parent, demonstrating that the ENU mutation was an allele of the murine Lyst gene. RT-PCR analyses revealed the skipping of exon 25 in Lystbg-grey mutants, which is predicted to cause a missense D2399E mutation and the loss of the following 77 amino acids encoded by exon 25 but leave the C-terminal end of the protein intact. Analysis of the genomic Lyst locus around exon 25 showed that the splice donor at the end of exon 25 showed a T-to-C transition point mutation. Western blot analysis suggests that the Lystbg-grey mutation causes instability of the LYST protein. Because the phenotype of Lystbg and Lystbg-grey mutants is indistinguishable, at least with respect to melanosomes and secretory granules in mast cells, the Lystbg-grey mutation defines a critical region for the stability of the murine LYST protein.
This is a preview of subscription content, log in via an institution to check access.
Similar content being viewed by others
References
Barbosa MD, Nguyen QA, Tchernev VT, Ashley JA, Detter JC, et al. (1996) Identification of the homologous beige and Chediak-Higashi syndrome genes. Nature 382:262–265
Barbosa MD, Barrat FJ, Tchernev VT, Nguyen QA, Mishra VS, et al. (1997) Identification of mutations in two major mRNA isoforms of the Chediak-Higashi syndrome gene in human and mouse. Hum Mol Genet 6: 1091–1098
Burkhardt JK, Wiebel FA, Hester S, Argon Y (1993) The giant organelles in beige and Chediak-Higashi fibroblasts are derived from late endosomes and mature lysosomes. J Exp Med 178: 1845–1856
Büssow H (1978) Schwann cell myelin ensheathing C.N.S. axons in the nerve fibre layer of the cat retina. J Neurocytol 7: 207–214
Certain S, Barrat F, Pastural E, Le Deist F, Goyo-Rivas J, et al. (2000) Protein truncation test of LYST reveals heterogenous mutations in patients with Chediak-Higashi syndrome. Blood 95: 979–983
Clark R, Griffiths GM (2003) Lytic granules, secretory lysosomes and disease. Curr Opin Immunol 15: 516–521
De Lozanne A (2003) The role of BEACH proteins in Dictyostelium. Traffic 4: 6–12
Fukai K, Oh J, Karim MA, Moore KJ, Kandil HH, et al. (1996) Homozygosity mapping of the gene for Chediak-Higashi syndrome to chromosome 1q42–q44 in a segment of conserved synteny that includes the mouse beige locus (bg). Am J Hum Genet 59: 620–624
Harris E, Wang N, Wu Wl WL, Weatherford A, De Lozanne A, et al. (2002) Dictyostelium LvsB mutants model the lysosomal defects associated with Chediak-Higashi syndrome. Mol Biol Cell 13: 656–669
Hearing VJ, Phillips P, Lutzner MA (1973) The fine structure of melanogenesis in coat color mutants of the mouse. J Ultrastruct Res 43: 88–106
Jackson IJ (1997) Homologous pigmentation mutations in human, mouse and other model organisms. Hum Mol Genet 6: 1613–1624
Karim MA, Nagle DL, Kandil HH, Burger J, Moore KJ, et al. (1997) Mutations in the Chediak-Higashi syndrome gene (CHS1) indicate requirement for the complete 3801 amino acid CHS protein. Hum Mol Genet 6: 1087–1089
Karim MA, Suzuki K, Fukai K, Oh J, Nagle DL, et al. (2002) Apparent genotype-phenotype correlation in childhood, adolescent, and adult Chediak-Higashi syndrome. Am J Med Genet 108: 16–22
Kent WJ (2002) BLAT—The BLAST-like alignment tool. Genome Res 12: 656–664
Kunieda T, Nakagiri M, Takami M, Ide H, Ogawa H (1999) Cloning of bovine LYST gene and identification of a missense mutation associated with Chediak-Higashi syndrome of cattle. Mamm Genome 10: 1146–1149
Mori M, Yamasaki K, Nakanishi S, Kitada K, Higuchi K, et al. (2003). A new beige mutant rat ACI/N-Lystbg-Kyo. Exp Anim 52: 31–36
Nagle DL, Karim MA, Woolf EA, Holmgren L, Bork P, et al. (1996) Identification and mutation analysis of the complete gene for Chediak-Higashi syndrome. Nat Genet 14: 307–311
Perou CM, Moore KJ, Nagle DL, Misumi DJ, Woolf EA, et al. (1996) Identification of the murine beige gene by YAC complementation and positional cloning. Nat Genet 13: 303–308
Perou CM, Pryor RJ, Naas TP, Kaplan J (1997a) The bg allele mutation is due to a LINE1 element retrotransposition. Genomics 42: 366–368
Perou CM, Leslie JD, Green W, Li L, Ward DM, Kaplan J (1997b) The Beige/Chediak-Higashi syndrome gene encodes a widely expressed cytosolic protein. J Biol Chem 272: 29790–29794
Shiflett SL, Kaplan J, Ward DM (2002) Chediak-Higashi Syndrome: a rare disorder of lysosomes and lysosome related organelles. Pigment Cell Res 15: 251–257
Silvers WK (1979) Beige. In The Coat Colors of Mice. A Model for Mammalian Gene Action and Interaction (New York: Springer Verlag), chap 6, pp 125–133 (also available online http://www.informatics.jax.org/wksilvers/)
Spritz RA (1998) Genetic defects in Chediak-Higashi syndrome and the beige mouse. J Clin Immunol 18: 97–105
Tchernev VT, Mansfield TA, Giot L, Kumar AM, Nandabalan K, et al. (2002) The Chediak-Higashi protein interacts with SNARE complex and signal transduction proteins. Mol Med 8: 56–64
Wang X, Herberg FW, Laue MM, Wullner C, Hu B, et al. (2000) Neurobeachin: A protein kinase A-anchoring, beige/Chediak-Higashi protein homolog implicated in neuronal membrane traffic. J Neurosci 20: 8551–8565
Ward DM, Shiflett SL, Huynh D, Vaughn MB, Prestwich G, et al. (2003) Use of expression constructs to dissect the functional domains of the CHS/beige protein: identification of multiple phenotypes. Traffic 4: 403–415
Acknowledgments
The authors thank M. Lindemann, G. Eversloh, M. Michels, and U. Schwaab for excellent technical support.
Author information
Authors and Affiliations
Corresponding author
Rights and permissions
About this article
Cite this article
Runkel, F., Büssow, H., Seburn, K.L. et al. Grey, a novel mutation in the murine Lyst gene, causes the beige phenotype by skipping of exon 25. Mamm Genome 17, 203–210 (2006). https://doi.org/10.1007/s00335-005-0015-1
Received:
Accepted:
Published:
Issue Date:
DOI: https://doi.org/10.1007/s00335-005-0015-1