Your search keyword '"Japanese domestic cat"' showing total 6 results

1. Novel Mutation in the Feline NPC2 Gene in Cats with Niemann–Pick Disease.

Author

Rakib, Tofazzal Md, Islam, Md Shafiqul, Uddin, Mohammad Mejbah, Rahman, Mohammad Mahbubur, Yabuki, Akira, Yamagami, Tetsushi, Morozumi, Motoji, Uchida, Kazuyuki, Maki, Shinichiro, Faruq, Abdullah Al, and Yamato, Osamu

Subjects

*CAT diseases, *NIEMANN-Pick diseases, *RECESSIVE genes, *GENETIC mutation, *PROTEIN stability, *MISSENSE mutation, *LYSOSOMAL storage diseases

Abstract

Simple Summary: Niemann–Pick disease (NP) type C is an autosomal recessive metabolic disorder caused by mutations in the NPC1 or NPC2 gene. It is characterized by cholesterol accumulation in the lysosomes and late endosomes. Herein, we studied the molecular basis of Siamese and Japanese domestic (JD) cats that were previously diagnosed with NP. Sanger sequencing was performed on all exons of the two genes using genomic DNA extracted from the paraffin-embedded tissues of these cats. As a result, a missense mutation (NPC2:c.376G>A, p.V126M) was identified as a candidate pathogenic mutation in both types of cats. Several pathogenicity and stability predictors showed that this mutation was deleterious and severely decreased NPC2 protein stability. The Siamese cat was homozygous and the JD cat was heterozygous for this mutation. No other exonic NPC2 mutations were detected in the JD cat; however, a homozygous splice variant (c.364-4C>T) was identified, which is not known to be associated with this disease. Niemann–Pick disease (NP) type C is an autosomal, recessive, and inherited neurovisceral genetic disorder characterized by the accumulation of unesterified cholesterol and glycolipids in cellular lysosomes and late endosomes, with a wide spectrum of clinical phenotypes. This study aimed to determine the molecular genetic alterations in two cases of felines with NP in Japan, a Siamese cat in 1989 and a Japanese domestic (JD) cat in 1998. Sanger sequencing was performed on 25 exons of the feline NPC1 gene and 4 exons of the feline NPC2 gene, using genomic DNA extracted from paraffin-embedded tissue specimens. The sequenced exons were compared with reference sequences retrieved from the GenBank database. The identified mutations and alterations were then analyzed using different prediction algorithms. No pathogenic mutations were found in feline NPC1; however, c.376G>A (p.V126M) was identified as a pathogenic mutation in the NPC2 gene. The Siamese cat was found to be homozygous for this mutation. The JD cat was heterozygous for the same mutation, but no other exonic NPC2 mutation was found. Furthermore, the JD cat had a homozygous splice variant (c.364-4C>T) in the NPC2 gene, which is not known to be associated with this disease. The NPC2:c.376G>A (p.V126M) mutation is the second reported pathogenic mutation in the feline NPC2 gene that may be present in the Japanese cat population. [ABSTRACT FROM AUTHOR]

Published

2023

2. Novel Mutation in the Feline NPC2 Gene in Cats with Niemann–Pick Disease

Author

Tofazzal Md Rakib, Md Shafiqul Islam, Mohammad Mejbah Uddin, Mohammad Mahbubur Rahman, Akira Yabuki, Tetsushi Yamagami, Motoji Morozumi, Kazuyuki Uchida, Shinichiro Maki, Abdullah Al Faruq, and Osamu Yamato

Subjects

Niemann–Pick disease type C, feline NPC2 gene, lysosomal storage disease, Siamese cat, Japanese domestic cat, Veterinary medicine, SF600-1100, Zoology, QL1-991

Abstract

Niemann–Pick disease (NP) type C is an autosomal, recessive, and inherited neurovisceral genetic disorder characterized by the accumulation of unesterified cholesterol and glycolipids in cellular lysosomes and late endosomes, with a wide spectrum of clinical phenotypes. This study aimed to determine the molecular genetic alterations in two cases of felines with NP in Japan, a Siamese cat in 1989 and a Japanese domestic (JD) cat in 1998. Sanger sequencing was performed on 25 exons of the feline NPC1 gene and 4 exons of the feline NPC2 gene, using genomic DNA extracted from paraffin-embedded tissue specimens. The sequenced exons were compared with reference sequences retrieved from the GenBank database. The identified mutations and alterations were then analyzed using different prediction algorithms. No pathogenic mutations were found in feline NPC1; however, c.376G>A (p.V126M) was identified as a pathogenic mutation in the NPC2 gene. The Siamese cat was found to be homozygous for this mutation. The JD cat was heterozygous for the same mutation, but no other exonic NPC2 mutation was found. Furthermore, the JD cat had a homozygous splice variant (c.364-4C>T) in the NPC2 gene, which is not known to be associated with this disease. The NPC2:c.376G>A (p.V126M) mutation is the second reported pathogenic mutation in the feline NPC2 gene that may be present in the Japanese cat population.

Published

2023

3. GM1 gangliosidosis in a Japanese domestic cat: a new variant identified in Hokkaido, Japan.

Author

Hiroshi UENO, Osamu YAMATO, Takeshi SUGIURA, Moeko KOHYAMA, Akira YABUKI, Kenjiro MIYOSHI, Kazuya MATSUDA, and Tsuyoshi UCHIDE

Subjects

SANDHOFF disease

Abstract

A male Japanese domestic cat with retarded growth in Hokkaido, Japan, showed progressive motor dysfunction, such as ataxia starting at 3 months of age and tremors, visual disorder and seizure after 4 months of age. Finally, the cat died of neurological deterioration at 9 months of age. Approximately half of the peripheral blood lymphocytes had multiple abnormal vacuoles. Magnetic resonance imaging showed bisymmetrical hyperintensity in the white matter of the parietal and occipital lobes in the forebrain on T2-weighted and fluid-attenuated inversion recovery images, and mild encephalatrophy of the olfactory bulbs and temporal lobes. The activity of lysosomal acid ß-galactosidase in leukocytes was negligible, resulting in the biochemical diagnosis of GM1 gangliosidosis. Histologically, swollen neurons characterized by accumulation of pale, slightly granular cytoplasmic materials were observed throughout the central nervous system. Dysmyelination or demyelination and gemistocytic astrocytosis were observed in the white matter. Ultrastructually, membranous cytoplasmic bodies were detected in the lysosomes of neurons. However, genetic analysis did not identify the c.1448G>C mutation, which is the single known mutation of feline GM1 gangliosidosis, suggesting that the cat was affected with a new variant of the feline disease. [ABSTRACT FROM AUTHOR]

Published

2016

4. Variation of amino acid sequences of serum amyloid a (SAA) and immunohistochemical analysis of amyloid a (AA) in Japanese domestic cats

Author

Kazuyuki Uchida, James K. Chambers, Hiroyuki Nakayama, Koichi Ohno, Takashi Tamamoto, Meina Tei, and Kenichi Watanabe

Subjects

Male, 0301 basic medicine, 040301 veterinary sciences, Inflammation, Biology, Cat Diseases, 0403 veterinary science, Pathogenesis, 03 medical and health sciences, Amyloid disease, Japan, AA amyloidosis, Pathology, medicine, Animals, Amino Acid Sequence, Serum amyloid A, Peptide sequence, Serum Amyloid A Protein, Full Paper, General Veterinary, Japanese domestic cat, fibril formation, Amyloidosis, DNA, 04 agricultural and veterinary sciences, medicine.disease, Molecular biology, SAA gene, 030104 developmental biology, Genes, Cats, Female, medicine.symptom

Abstract

Amyloid A (AA) amyloidosis, a fatal systemic amyloid disease, occurs secondary to chronic inflammatory conditions in humans. Although persistently elevated serum amyloid A (SAA) levels are required for its pathogenesis, not all individuals with chronic inflammation necessarily develop AA amyloidosis. Furthermore, many diseases in cats are associated with the elevated production of SAA, whereas only a small number actually develop AA amyloidosis. We hypothesized that a genetic mutation in the SAA gene may strongly contribute to the pathogenesis of feline AA amyloidosis. In the present study, genomic DNA from four Japanese domestic cats (JDCs) with AA amyloidosis and from five without amyloidosis was analyzed using polymerase chain reaction (PCR) amplification and direct sequencing. We identified the novel variation combination of 45R-51A in the deduced amino acid sequences of four JDCs with amyloidosis and five without. However, there was no relationship between amino acid variations and the distribution of AA amyloid deposits, indicating that differences in SAA sequences do not contribute to the pathogenesis of AA amyloidosis. Immunohistochemical analysis using antisera against the three different parts of the feline SAA protein-i.e., the N-terminal, central, and C-terminal regions-revealed that feline AA contained the C-terminus, unlike human AA. These results indicate that the cleavage and degradation of the C-terminus are not essential for amyloid fibril formation in JDCs.

Published

2018

5. GM1 gangliosidosis in a Japanese domestic cat: a new variant identified in Hokkaido, Japan

Author

Osamu Yamato, Kazuya Matsuda, Moeko Kohyama, Tsuyoshi Uchide, Kenjiro Miyoshi, Takeshi Sugiura, Hiroshi Ueno, and Akira Yabuki

Subjects

Male, Pathology, medicine.medical_specialty, Ataxia, 040301 veterinary sciences, Central nervous system, β-galactosidase deficiency, Gangliosidosis, Biology, Cat Diseases, 0403 veterinary science, White matter, Japan, feline GM1 gangliosidosis, Internal medicine, 0502 economics and business, Internal Medicine, Lysosomal storage disease, medicine, Animals, Gangliosidosis, GM1, Japanese domestic cat, General Veterinary, 05 social sciences, 04 agricultural and veterinary sciences, Note, medicine.disease, Hyperintensity, medicine.anatomical_structure, Endocrinology, lysosomal storage disease, Forebrain, Cats, 050211 marketing, Astrocytosis, medicine.symptom

Abstract

A male Japanese domestic cat with retarded growth in Hokkaido, Japan, showed progressive motor dysfunction, such as ataxia starting at 3 months of age and tremors, visual disorder and seizure after 4 months of age. Finally, the cat died of neurological deterioration at 9 months of age. Approximately half of the peripheral blood lymphocytes had multiple abnormal vacuoles. Magnetic resonance imaging showed bisymmetrical hyperintensity in the white matter of the parietal and occipital lobes in the forebrain on T2-weighted and fluid-attenuated inversion recovery images, and mild encephalatrophy of the olfactory bulbs and temporal lobes. The activity of lysosomal acid β-galactosidase in leukocytes was negligible, resulting in the biochemical diagnosis of GM1 gangliosidosis. Histologically, swollen neurons characterized by accumulation of pale, slightly granular cytoplasmic materials were observed throughout the central nervous system. Dysmyelination or demyelination and gemistocytic astrocytosis were observed in the white matter. Ultrastructually, membranous cytoplasmic bodies were detected in the lysosomes of neurons. However, genetic analysis did not identify the c.1448G>C mutation, which is the single known mutation of feline GM1 gangliosidosis, suggesting that the cat was affected with a new variant of the feline disease.

Published

2016

6. Variation of amino acid sequences of serum amyloid a (SAA) and immunohistochemical analysis of amyloid a (AA) in Japanese domestic cats.

Author

Tei M, Uchida K, Chambers JK, Watanabe KI, Tamamoto T, Ohno K, and Nakayama H

Subjects

Amino Acid Sequence, Amyloidosis veterinary, Animals, Cat Diseases genetics, Cats blood, DNA genetics, Female, Genes genetics, Japan, Male, Serum Amyloid A Protein analysis, Serum Amyloid A Protein immunology, Cats genetics, Serum Amyloid A Protein genetics

Abstract

Amyloid A (AA) amyloidosis, a fatal systemic amyloid disease, occurs secondary to chronic inflammatory conditions in humans. Although persistently elevated serum amyloid A (SAA) levels are required for its pathogenesis, not all individuals with chronic inflammation necessarily develop AA amyloidosis. Furthermore, many diseases in cats are associated with the elevated production of SAA, whereas only a small number actually develop AA amyloidosis. We hypothesized that a genetic mutation in the SAA gene may strongly contribute to the pathogenesis of feline AA amyloidosis. In the present study, genomic DNA from four Japanese domestic cats (JDCs) with AA amyloidosis and from five without amyloidosis was analyzed using polymerase chain reaction (PCR) amplification and direct sequencing. We identified the novel variation combination of 45R-51A in the deduced amino acid sequences of four JDCs with amyloidosis and five without. However, there was no relationship between amino acid variations and the distribution of AA amyloid deposits, indicating that differences in SAA sequences do not contribute to the pathogenesis of AA amyloidosis. Immunohistochemical analysis using antisera against the three different parts of the feline SAA protein-i.e., the N-terminal, central, and C-terminal regions-revealed that feline AA contained the C-terminus, unlike human AA. These results indicate that the cleavage and degradation of the C-terminus are not essential for amyloid fibril formation in JDCs.

Published

2018