Your search keyword '"Masao Ono"' showing total 6 results

1. Presumptive role of 129 strain-derivedSle16locus in rheumatoid arthritis in a new mouse model with Fcγ receptor type IIb-deficient C57BL/6 genetic background

Author

Sachiko Hirose, Toshiyuki Takai, Katsuko Sudo, Keiko Nishikawa, Masao Ono, Shozo Izui, Naomi Ohtsuji, Mareki Ohtsuji, Qingshun Lin, Rong Hou, Toshikazu Shirai, Aya Sato-Hayashizaki, Hiroyuki Nishimura, and Hiromichi Tsurui

Subjects

C57BL/6, Autoimmune disease, Genetics, 0303 health sciences, biology, Immunology, Congenic, Arthritis, Locus (genetics), FCGR2B, biology.organism_classification, medicine.disease, Molecular biology, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, medicine, Immunology and Allergy, Pharmacology (medical), Gene polymorphism, Gene, 030304 developmental biology, 030215 immunology

Abstract

Objective Fcγ receptor type IIb (FcγRIIb) is a major negative regulator of B cells, and the lack of FcγRIIb expression has been reported to induce systemic lupus erythematosus (SLE) in mice of the C57BL/6 (B6) genetic background. The 129 strain–derived Sle16 locus on the telomeric region of chromosome 1 including polymorphic Fcgr2b confers the predisposition to systemic autoimmunity when present on the B6 background. We undertook this study to examine the effect of the Sle16 locus on autoimmune disease in FcγRIIb-deficient B6 mice. Methods We established 2 lines of FcγRIIb-deficient B6 congenic mouse strains (KO1 and KO2) by selective backcrossing of the originally constructed FcγRIIb-deficient mice on a hybrid (129 × B6) background into a B6 background. Although both lack FcγRIIb expression, the KO1 and KO2 strains carry different lengths of the 129 strain–derived telomeric chromosome 1 segment flanked to the null-mutated Fcgr2b gene; the KO1 strain carries a 129 strain–derived ∼6.3-Mb interval distal from the null-mutated Fcgr2b gene within the Sle16 locus, while this interval in the KO2 strain is of B6 origin. Results Unexpectedly, both strains failed to develop SLE; instead, the KO1 strain, but not the KO2 strain, spontaneously developed severe rheumatoid arthritis (RA) with an incidence reaching >90% at age 12 months. Conclusion The current study shows evidence that the epistatic interaction between the Fcgr2b-null mutation and a polymorphic gene(s) in the 129 strain–derived interval located in the distal Sle16 locus contributes to RA susceptibility in a new mouse model with the B6 genetic background, although the participation of other genetic polymorphisms cannot be totally excluded.

Published

2011

2. Cappuccino mutation in an autoimmune-prone strain of mice suggests a role of platelet function in the progression of immune complex crescentic glomerulonephritis

Author

Hiroaki Komori, Masao Ono, Shoko Iwaki, Norimasa Arita, Kazutaka Maeyama, Kan Saiga, Takaaki Hato, Minako Yoshida, Masato Nose, Hiroshi Furukawa, Kyuichi Nemoto, Toshiyuki Niiya, Miho Terada, and Takahito Tsubaki

Subjects

Blood Platelets, Positional cloning, Renal glomerulus, Immunoblotting, Molecular Sequence Data, Immunology, Mutant, Vesicular Transport Proteins, Biology, medicine.disease_cause, Autoimmune Diseases, Blood Urea Nitrogen, Mice, Glomerulonephritis, Rheumatology, Glomerulopathy, medicine, Animals, Immunology and Allergy, Pharmacology (medical), Platelet, Amino Acid Sequence, DNA Primers, Mutation, medicine.disease, Mice, Mutant Strains, Immune complex, Blood Cell Count, Phenotype

Abstract

Objective Crescent formation in the renal glomerulus is a typical manifestation of progressive glomerulopathy associated with fatal renal failure; therefore, its prevention is of clinical importance. Little is known about the pathogenic mechanism for crescent formation. This study was undertaken in an attempt to identify the events that are critical for crescent formation in immune complex crescentic glomerulonephritis (CGN) by analyzing a novel mutant strain of mice. Methods A spontaneous mutant strain of mice was isolated from the autoimmune-prone strain EOD, which stably develops fatal CGN. The mutant phenotypes were assessed histopathologically, hematologically, and immunologically. The mutation was searched for with positional cloning using microsatellite markers. Results Compared with wild-type EOD (WT-EOD) mice, mutant EOD (mut-EOD) mice showed marked improvement in CGN in conjunction with an improvement in spontaneous mortality. In WT-EOD mice, an inverse correlation between blood urea nitrogen concentration and blood platelet count and massive accumulation of platelets in the glomerulus were evident, suggesting that an accumulation of platelets in the glomerulus contributes to the progression of CGN. The mutant platelets showed an abnormal aggregation in response to collagen and thrombin, associated with a bleeding tendency in mut-EOD mice. Genetic analysis revealed a deleterious mutation in the cappuccino gene (cno), which encodes a protein that belongs to a complex called the biogenesis of lysosome-related organelle complex 1 and is profoundly involved in platelet function. Morphologic examination revealed a partial defect in dense body formation in the δ-granule of platelets. Conclusion The present findings suggest that platelet functions have a critical role in crescent formation in autoimmune GN.

Published

2006

3. Genetic basis of tissue specificity of vasculitis in MRL/lpr mice

Author

Mitsuko R. Ito, Masao Ono, Masato Nose, Shiro Mori, Yusuke Nakamura, Miho Terada, Ling-Min Lu, Yoshimi Nozaki, Tatsuhiko Miyazaki, Morikazu Onji, Akihiro Yamada, Kazuya Hata, and Shuichi Nakatsuru

Subjects

Male, Vasculitis, Mice, Inbred MRL lpr, Systemic disease, Pathology, medicine.medical_specialty, Quantitative Trait Loci, Immunology, Locus (genetics), Biology, Quantitative trait locus, urologic and male genital diseases, Polymerase Chain Reaction, Pathogenesis, Mice, Rheumatology, immune system diseases, medicine, Animals, Immunology and Allergy, Genetic Predisposition to Disease, Pharmacology (medical), skin and connective tissue diseases, Aorta, Crosses, Genetic, Mice, Inbred C3H, Chromosome, DNA, medicine.disease, Disease Models, Animal, Chromosome 4, Organ Specificity, Female, Lod Score, Microsatellite Repeats, Systemic vasculitis

Abstract

Objective To clarify the mode of inheritance of the tissue distribution of vasculitis in MRL/Mp-lpr/lpr (MRL/lpr) lupus-prone mice and to identify the susceptibility loci. Methods Vasculitis in individual MRL/lpr, C3H/HeJ-lpr/lpr (C3H/lpr), (MRL/lpr × C3H/lpr)F1, and (MRL/lpr × C3H/lpr)F2 intercross mice was analyzed by histopathologic grading of main branches of the aorta and of medium-sized arteries in the lower limbs. Genomic DNA samples from F2 intercross mice were examined by simple sequence-length polymorphism analysis, and the polymorphic microsatellite markers highly associated with vasculitis in each tissue were determined as vasculitis susceptibility loci. Results A susceptibility locus with significant linkage to vasculitis of main branches of the aorta was mapped on chromosome 4 at D4Mit213 (map position 13.3cM) selectively in males, while vasculitis of medium-sized arteries in the lower limbs was mapped to different chromosomes: at D8Mit31 on chromosome 8 (map position 33.0) selectively in females and at D5Mit36 on chromosome 5 (map position 65.0). All of these were different from the previously defined loci governing susceptibility to vasculitis involving the kidneys. Conclusion Systemic vasculitis in MRL/lpr mice is genetically controlled with cumulative effects of multiple gene loci, each of which has tissue specificity.

Published

2003

4. Cappuccino mutation in an autoimmune‐prone strain of mice suggests a role of platelet function in the progression of immune complex crescentic glomerulonephritis.

Author

Minako Yoshida, Kan Saiga, Takaaki Hato, Shoko Iwaki, Toshiyuki Niiya, Norimasa Arita, Hiroaki Komori, Takahito Tsubaki, Hiroshi Furukawa, Miho Terada, Kazutaka Maeyama, Kyuichi Nemoto, Masato Nose, and Masao Ono

Subjects

GLOMERULONEPHRITIS, IMMUNE complex diseases, KIDNEY glomerulus diseases, GENETIC mutation, BLOOD platelets, LABORATORY mice

Abstract

Crescent formation in the renal glomerulus is a typical manifestation of progressive glomerulopathy associated with fatal renal failure; therefore, its prevention is of clinical importance. Little is known about the pathogenic mechanism for crescent formation. This study was undertaken in an attempt to identify the events that are critical for crescent formation in immune complex crescentic glomerulonephritis (CGN) by analyzing a novel mutant strain of mice.A spontaneous mutant strain of mice was isolated from the autoimmune‐prone strain EOD, which stably develops fatal CGN. The mutant phenotypes were assessed histopathologically, hematologically, and immunologically. The mutation was searched for with positional cloning using microsatellite markers.Compared with wild‐type EOD (WT‐EOD) mice, mutant EOD (mut‐EOD) mice showed marked improvement in CGN in conjunction with an improvement in spontaneous mortality. In WT‐EOD mice, an inverse correlation between blood urea nitrogen concentration and blood platelet count and massive accumulation of platelets in the glomerulus were evident, suggesting that an accumulation of platelets in the glomerulus contributes to the progression of CGN. The mutant platelets showed an abnormal aggregation in response to collagen and thrombin, associated with a bleeding tendency in mut‐EOD mice. Genetic analysis revealed a deleterious mutation in the cappuccino gene (cno), which encodes a protein that belongs to a complex called the biogenesis of lysosome‐related organelle complex 1 and is profoundly involved in platelet function. Morphologic examination revealed a partial defect in dense body formation in the δ‐granule of platelets.The present findings suggest that platelet functions have a critical role in crescent formation in autoimmune GN. [ABSTRACT FROM AUTHOR]

Published

2006

5. Accelerating effect of an MRL gene locus on the severity and onset of arthropathy in DBA/1 mice.

Author

Hisashi Oishi, Tatsuhiko Miyazaki, Shinichi Mizuki, Junji Kamogawa, Ling‐Min Lu, Takahito Tsubaki, Norimasa Arita, Masao Ono, Haruyasu Yamamoto, and Masato Nose

Subjects

ARTHRITIS, JOINT diseases, HISTOPATHOLOGY, LABORATORY animals, MICE

Abstract

To analyze the influence of the genetic background of an arthritis‐prone strain of mice, MRL, on the spontaneous development of arthropathy in DBA/1 mice, which histopathologically resembles enthesopathy in humans, and to clarify the strain‐specific gene loci and their interactions that confer susceptibility to arthropathy.MRL, DBA/1, (MRL × DBA/1)F1, and (MRL × DBA/1)F2 intercross mice were prepared, and the severity and onset of arthropathy of the ankle joints in individual mice were quantified (0–3 and 0–5 scale, respectively). A genome‐wide scan of 271 male F2 intercross mice with polymorphic microsatellite markers was performed. Only male DBA/1, (MRL × DBA/1)F1, and (MRL × DBA/1)F2 mice developed arthropathy. The macroscopic and histopathologic findings of arthropathy in the F2 mice were similar to those in the parental DBA/1 mice, but the onset was significantly earlier. In the quantitative trait locus analysis of male F2 mice, 1 susceptibility locus for both the severity and early onset of the disease in the region of an MRL allele, Amd1, was located at marker D10Mit259 (map position 40.0 cM), which was common to 1 of the sialadenitis susceptibility loci in MRL mice, Asm1. Another susceptibility locus for the severity and early onset of arthropathy in the region of a DBA allele, Amd2, was located at D3Mit46 (29.5 cM). These loci manifested an additive effect on the development of arthropathy. Arthropathy in DBA/1 mice is under the control of an allelic combination of gene loci, one of which is common to the locus for sialadenitis in MRL/MpJ‐lpr/lpr mice. [ABSTRACT FROM AUTHOR]

Published

2005

6. Genetic basis of tissue specificity of vasculitis in MRL/lpr mice.

Author

Akihiro Yamada, Tatsuhiko Miyazaki, Ling-Min Lu, Masao Ono, Mitsuko R. Ito, Miho Terada, Shiro Mori, Kazuya Hata, Yoshimi Nozaki, Shuichi Nakatsuru, Yusuke Nakamura, Morikazu Onji, and Masato Nose

Subjects

VASCULITIS, GENETIC polymorphisms, MICE, ARTERIES, LEG, DNA

Abstract

To clarify the mode of inheritance of the tissue distribution of vasculitis in MRL/Mp-lpr/lpr (MRL/lpr) lupus-prone mice and to identify the susceptibility loci. Vasculitis in individual MRL/lpr, C3H/HeJ-lpr/lpr (C3H/lpr), (MRL/lpr × C3H/lpr)F1, and (MRL/lpr × C3H/lpr)F2 intercross mice was analyzed by histopathologic grading of main branches of the aorta and of medium-sized arteries in the lower limbs. Genomic DNA samples from F2 intercross mice were examined by simple sequence-length polymorphism analysis, and the polymorphic microsatellite markers highly associated with vasculitis in each tissue were determined as vasculitis susceptibility loci. A susceptibility locus with significant linkage to vasculitis of main branches of the aorta was mapped on chromosome 4 at D4Mit213 (map position 13.3cM) selectively in males, while vasculitis of medium-sized arteries in the lower limbs was mapped to different chromosomes: at D8Mit31 on chromosome 8 (map position 33.0) selectively in females and at D5Mit36 on chromosome 5 (map position 65.0). All of these were different from the previously defined loci governing susceptibility to vasculitis involving the kidneys. Systemic vasculitis in MRL/lpr mice is genetically controlled with cumulative effects of multiple gene loci, each of which has tissue specificity. [ABSTRACT FROM AUTHOR]

Published

2003