Your search keyword '"Welle, Monika M."' showing total 4 results

1. A Large Deletion in the NSDHL Gene in Labrador Retrievers with a Congenital Cornification Disorder.

Author

Bauer, Anina, De Lucia, Michela, Jagannathan, Vidhya, Mezzalira, Giorgia, Casal, Margret L., Welle, Monika M., and Leeb, Tosso

Subjects

*LABRADOR retriever, *X chromosome, *CONGENITAL disorders

Abstract

In heterozygous females affected by an X-linked skin disorder, lesions often appear in a characteristic pattern, the so-called Blaschko's lines. We investigated a female Labrador Retriever and her crossbred daughter, which both showed similar clinical lesions that followed Blaschko's lines. The two male littermates of the affected daughter had died at birth, suggesting a monogenic X-chromosomal semidominant mode of inheritance. Whole genome sequencing of the affected daughter, and subsequent automated variant filtering with respect to 188 nonaffected control dogs of different breeds, revealed 332 heterozygous variants on the X-chromosome private to the affected dog. None of these variants was proteinchanging. By visual inspection of candidate genes located on the X-chromosome, we identified a large deletion in the NSDHL gene, encoding NAD(P) dependent steroid dehydrogenase-like, a 3b-hydroxysteroid dehydrogenase involved in cholesterol biosynthesis. The deletion spanned .14 kb, and included the last three exons of the NSDHL gene. By PCR and fragment length analysis, we confirmed the presence of the variant in both affected dogs, and its absence in 50 control Labrador Retrievers. Variants in the NSDHL gene cause CHILD syndrome in humans, and the bare patches (Bpa) and striated (Str) phenotypes in mice. Taken together, our genetic data and the known role of NSDHL in X-linked skin disorders strongly suggest that the identified structural variant in the NSDHL gene is causative for the phenotype in the two affected dogs. [ABSTRACT FROM AUTHOR]

Published

2017

2. A Nonsense Variant in the ST14 Gene in Akhal-Teke Horses with Naked Foal Syndrome.

Author

Bauer, Anina, Hiemesch, Theresa, Jagannathan, Vidhya, Neuditschko, Markus, Bachmann, Iris, Rieder, Stefan, Mikko, Sofia, Penedo, M. Cecilia, Tarasova, Nadja, Vitková, Martina, Sirtori, Nicolò, Roccabianca, Paola, Leeb, Tosso, and Welle, Monika M.

Subjects

*SKIN disease genetics, *PHENOTYPES, *HORSES, *GENETICS

Abstract

Naked foal syndrome (NFS) is a genodermatosis in the Akhal-Teke horse breed. We provide the first scientific description of this phenotype. Affected horses have almost no hair and show a mild ichthyosis. So far, all known NFS affected horses died between a few weeks and 3 yr of age. It is not clear whether a specific pathology caused the premature deaths. NFS is inherited as a monogenic autosomal recessive trait. We mapped the disease causing genetic variant to two segments on chromosomes 7 and 27 in the equine genome. Whole genome sequencing of two affected horses, two obligate carriers, and 75 control horses from other breeds revealed a single nonsynonymous genetic variant on the chromosome 7 segment that was perfectly associated with NFS. The affected horses were homozygous for ST14:c.388G.T, a nonsense variant that truncates .80% of the open reading frame of the ST14 gene (p.Glu130). The variant leads to partial nonsense-mediated decay of the mutant transcript. Genetic variants in the ST14 gene are responsible for autosomal recessive congenital ichthyosis 11 in humans. Thus, the identified equine ST14:c.388G.T variant is an excellent candidate causative variant for NFS, and the affected horses represent a large animal model for a known human genodermatosis. Our findings will enable genetic testing to avoid the nonintentional breeding of NFS-affected foals. [ABSTRACT FROM AUTHOR]

Published

2017

3. A Splice Defect in the EDA Gene in Dogs with an X-Linked Hypohidrotic Ectodermal Dysplasia (XLHED) Phenotype.

Author

Waluk, Dominik P., Galichet, Arnaud, Müller, Eliane J., Welle, Monika M., Jagannathan, Vidhya, Drögemüller, Cord, Leeb, Tosso, Zur, Gila, and Kaufmann, Ronnie

Subjects

*DOGS, *RNA sequencing, *RNA splicing

Abstract

X-linked hypohidrotic ectodermal dysplasia (XLHED) caused by variants in the EDA gene represents the most common ectodermal dysplasia in humans. We investigated three male mixed-breed dogs with an ectodermal dysplasia phenotype characterized by marked hypotrichosis and multifocal complete alopecia, almost complete absence of sweat and sebaceous glands, and altered dentition with missing and abnormally shaped teeth. Analysis of SNP chip genotypes and whole genome sequence data from the three affected dogs revealed that the affected dogs shared the same haplotype on a large segment of the X-chromosome, including the EDA gene. Unexpectedly, the whole genome sequence data did not reveal any nonsynonymous EDA variant in the affected dogs. We therefore performed an RNA-seq experiment on skin biopsies to search for changes in the transcriptome. This analysis revealed that the EDA transcript in the affected dogs lacked 103 nucleotides encoded by exon 2. We speculate that this exon skipping is caused by a genetic variant located in one of the large introns flanking this exon, which was missed by whole genome sequencing with the illumina short read technology. The altered EDA transcript splicing most likely causes the observed ectodermal dysplasia in the affected dogs. These dogs thus offer an excellent opportunity to gain insights into the complex splicing processes required for expression of the EDA gene, and other genes with large introns. [ABSTRACT FROM AUTHOR]

Published

2016

4. An Intronic MBTPS2 Variant Results in a Splicing Defect in Horses with Brindle Coat Texture.

Author

Wiedemar, Natalie, Dietrich, Joëlle, Jagannathan, Vidhya, Drögemüller, Michaela, Leeb, Tosso, Murgiano, Leonardo, Waluk, Dominik P., Galichet, Arnaud, Balmer, Pierre, Müller, Eliane J., Welle, Monika M., Roosje, Petra, Towers, Rachel, Druet, Tom, and Penedo, M. Cecilia

Subjects

*HORSE diseases, *PHENOTYPES, *DERMATOLOGY

Abstract

We investigated a family of horses exhibiting irregular vertical stripes in their hair coat texture along the neck, back, hindquarters, and upper legs. This phenotype is termed “brindle” by horse breeders. We propose the term “brindle 1 (BR1)” for this specific form of brindle. In some BR1 horses, the stripes were also differentially pigmented. Pedigree analyses were suggestive of a monogenic X-chromosomal semidominant mode of inheritance. Haplotype analyses identified a 5 Mb candidate region on chromosome X. Whole genome sequencing of four BR1 and 60 nonbrindle horses identified 61 private variants in the critical interval, none of them located in an exon of an annotated gene. However, one of the private variants was close to an exon/intron boundary in intron 10 of the MBTPS2 gene encoding the membrane bound transcription factor peptidase, site 2 (c.1437+4T>C). Different coding variants in this gene lead to three related genodermatoses in human patients. We therefore analyzed MBTPS2 transcripts in skin, and identified an aberrant transcript in a BR1 horse, which lacked the entire exon 10 and parts of exon 11. The MBTPS2:c1437+4T>C variant showed perfect cosegregation with the brindle phenotype in the investigated family, and was absent from 457 control horses of diverse breeds. Altogether, our genetic data, and previous knowledge on MBTPS2 function in the skin, suggest that the identified MBTPS2 intronic variant leads to partial exon skipping, and causes the BR1 phenotype in horses. [ABSTRACT FROM AUTHOR]

Published

2016