Your search keyword '"Mice, Mutant Strains physiology"' showing total 9 results

1. Mouse model for Usher syndrome: linkage mapping suggests homology to Usher type I reported at human chromosome 11p15.

Author

Heckenlively JR, Chang B, Erway LC, Peng C, Hawes NL, Hageman GS, and Roderick TH

Subjects

Animals, Deafness pathology, Deafness physiopathology, Disease Models, Animal, Ear, Inner pathology, Genes, Recessive, Humans, Mice, Mice, Inbred C57BL, Mice, Mutant Strains anatomy & histology, Mice, Mutant Strains physiology, Retinal Degeneration pathology, Retinal Degeneration physiopathology, Rod Cell Outer Segment ultrastructure, Syndrome, Chromosomes, Human, Pair 11, Deafness genetics, Mice, Mutant Strains genetics, Retinal Degeneration genetics

Abstract

Usher syndrome is a group of diseases with autosomal recessive inheritance, congenital hearing loss, and the development of retinitis pigmentosa, a progressive retinal degeneration characterized by night blindness and visual field loss over several decades. The causes of Usher syndrome are unknown and no animal models have been available for study. Four human gene sites have been reported, suggesting at least four separate forms of Usher syndrome. We report a mouse model of type I Usher syndrome, rd5, whose linkage on mouse chromosome 7 to Hbb and tub has homology to human Usher I reported on human chromosome 11p15. The electroretinogram in homozygous rd5/rd5 mouse is never normal with reduced amplitudes that extinguish by 6 months. Auditory-evoked response testing demonstrates increased hearing thresholds more than control at 3 weeks of about 30 decibels (dB) that worsen to about 45 dB by 6 months.

Published

1995

2. Expression of a Pim-1 transgene accelerates lymphoproliferation and inhibits apoptosis in lpr/lpr mice.

Author

Möröy T, Grzeschiczek A, Petzold S, and Hartmann KU

Subjects

Animals, Antigens, Surface physiology, Autoimmune Diseases genetics, CD4-Positive T-Lymphocytes cytology, CD8 Antigens analysis, Dexamethasone pharmacology, Lymph Nodes cytology, Mice, Mice, Inbred C57BL, Mice, Transgenic, Protein-Tyrosine Kinases physiology, Proto-Oncogene Proteins c-pim-1, T-Lymphocyte Subsets cytology, fas Receptor, Apoptosis drug effects, Hematopoiesis, Lymphoproliferative Disorders genetics, Mice, Mutant Strains physiology, Protein Serine-Threonine Kinases, Proto-Oncogene Proteins physiology

Abstract

Transgenic mice expressing the Pim-1 kinase are predisposed to develop T-cell lymphomas with a long latency period of about 7-9 months. However, the exact functional basis of the oncogenic activity of Pim-1 remains obscure. C57BL/6 mice homozygous for the lpr mutation develop a well-described lymphoproliferative syndrome at about 26-30 weeks of age. This syndrome is characterized mainly by the accumulation of abnormal T cells in lymph nodes because of the lack of Fas receptor-induced apoptosis. We find that backcross of E mu-Pim-1 transgenics (mice with a transgene that carries the mouse Pim-1 gene under the transcriptional control of the immunoglobulin heavy chain gene enhancer E mu) into lpr/lpr mice results in strong acceleration of lymphoproliferation and dramatic enlargement of lymph nodes. In addition, we show here that cultured lymph node cells from E mu-Pim-1 lpr/lpr mice are rescued from rapid apoptosis that normally occurs in nontransgenic lpr cells in vitro. We also present evidence that CD4+/CD8+ double-positive thymocytes from lpr/lpr mice are sensitive to dexamethasone-induced apoptosis, although lpr/lpr mice lack the Fas receptor. In contrast, E mu-Pim-1 lpr/lpr animals show considerable protection from dexamethasone-induced apoptosis. These results show that Pim-1 can strongly accelerate lymphoproliferation through inhibition of apoptosis and thereby provide first insight into the functional basis for the oncogenic activity of Pim-1.

Published

1993

3. The effects of dietary restriction on immune function and development of autoimmune disease in BXSB mice.

Author

Kubo C, Gajar A, Johnson BC, and Good RA

Subjects

Age Factors, Animals, Antibodies, Antinuclear immunology, Antigen-Antibody Complex metabolism, Antigens, Surface analysis, B-Lymphocytes immunology, Cytotoxicity, Immunologic, Interleukin-2 biosynthesis, Isoantigens, Leukocyte Count, Longevity, Lymphocyte Activation, Lymphocyte Culture Test, Mixed, Male, Membrane Glycoproteins analysis, Mice, Organ Size, Receptors, Antigen, B-Cell analysis, Thy-1 Antigens, Autoimmune Diseases physiopathology, Energy Intake, Mice, Mutant Strains physiology

Abstract

Chronic energy intake restriction (CEIR) prolonged the median life span and inhibited autoimmunity and development of autoimmune disease in BXSB mice, as has been established for mice of several other autoimmune-prone, short-lived strains. Whether imposed just after weaning or delayed until manifestations of disease had appeared, CEIR inhibited or reversed development of autoimmunity and immune complex-based renal disease in male BXSB mice. CEIR also prevented the formation of anti-DNA antibodies and prevented the increase in circulating immune complex levels that is typically observed in male mice of this strain. Moreover, CEIR inhibited development of splenomegaly and prevented the normal age-associated decline of a number of immunological functions, including interleukin 2 production, cell-mediated cytotoxic responses, and mixed lymphocyte reactivity. The observed improvement in cell-mediated immune responses was attributed largely to the capacity of CEIR to inhibit development of the splenomegaly that occurs concomitant with expansion of a non-T, non-B lymphoid cell population. These findings emphasize that CEIR, even when imposed relatively late in life in BXSB mice, can influence expression of autoimmunities and autoimmune diseases of different genetic origins and presumed pathogenetic bases.

Published

1992

4. Calcium-binding protein, parvalbumin, is reduced in mutant mammalian muscle with abnormal contractile properties.

Author

Stuhlfauth I, Reininghaus J, Jockusch H, and Heizmann CW

Subjects

Animals, Isoelectric Point, Mice, Molecular Weight, Muscle Contraction, Muscles ultrastructure, Mutation, Parvalbumins deficiency, Parvalbumins genetics, Peptide Fragments analysis, Mice, Mutant Strains physiology, Muscle Proteins physiology, Parvalbumins physiology

Abstract

To elucidate the biochemical basis of hereditary muscle diseases in an experimental mammal, we performed polypeptide analyses on skeletal muscles of neuromuscular mutants of the mouse. In one of these, "arrested development of righting response" (adr), the concentration of the soluble Ca2+-binding protein parvalbumin was drastically reduced in comparison to wild type. This reduction was not an unspecific consequence of muscle disease, as it was not observed in two other neuromuscular mouse mutants, "wobbler" (wr) and "motor endplate disease" (med or medjo). Isometric twitches of adr muscle had only slightly prolonged contraction and half-relaxation times, yet long-lasting after-contractions were observed upon repeated (20-100 Hz) direct stimulation. Thus, parvalbumin may be mainly involved in the relaxation after tetanic contraction of fast-twitch fibers.

Published

1984

5. The Gy mutation: another cause of X-linked hypophosphatemia in mouse.

Author

Lyon MF, Scriver CR, Baker LR, Tenenhouse HS, Kronick J, and Mandla S

Subjects

Alkaline Phosphatase blood, Animals, Behavior, Animal physiology, Biological Transport, Body Weight, Bone Development, Calcium metabolism, Chromosome Mapping, Creatinine blood, Female, Genetic Linkage, Hypophosphatemia, Familial genetics, Hypophosphatemia, Familial physiopathology, Kidney physiopathology, Male, Mice, Mutant Strains physiology, Microvilli metabolism, Motor Activity, Mutation, Parathyroid Hormone blood, Phenotype, Phosphorus metabolism, Sodium metabolism, Hypophosphatemia, Familial veterinary, Mice genetics, X Chromosome

Abstract

An X-linked dominant mutation (gyro, gene symbol Gy) in the laboratory mouse causes hypophosphatemia, rickets/osteomalacia, circling behavior, inner ear abnormalities, and sterility in males and a milder phenotype in females. Gy maps closely (crossover value 0.4-0.8%) to another X-linked gene (Hyp) that also causes hypophosphatemia in the mouse. Gy and Hyp genes have similar quantitative expression in serum phosphorus values, renal excretion of phosphate, and impairment of Na+/phosphate cotransport by renal brush-border membrane vesicles. These findings indicate that independent translation products of two X-linked genes serve phosphate transport in mouse kidney and thereby control phosphate content of extracellular fluid. The Gy translation product, unlike the Hyp product, is also expressed in the inner ear. These findings have implications for our understanding of the human counterpart known as "X-linked hypophosphatemia."

Published

1986

6. Partitioning of bone marrow into stem cell regulatory domains.

Author

Maloney MA, Lamela RA, Banda MJ, and Patt HM

Subjects

Animals, Colony-Forming Units Assay, Hematopoiesis, Male, Mice, Mice, Mutant Strains physiology, Radiation Chimera, Bone Marrow Cells, Hematopoietic Stem Cells cytology

Abstract

To examine the hypothesis that bone marrow consists of discrete stem cell regulatory volumes or domains, we studied spleen colony-forming unit (CFU-S) population growth kinetics in unirradiated WBB6F1-W/Wv mice receiving various doses of +/+ bone marrow cells. Assay of femoral marrow CFU-S content in the eight recipient dose groups revealed a family of growth curves having an initial dose-independent exponential phase and a subsequent dose-dependent deceleration phase. CFU-S content at the growth transition (inflection point) was not a simple linear function of inoculum dose but was shown rather to reflect a random distribution of initially seeded donor CFU-S in discrete volumes of recipient bone marrow. The inoculum dose resulting in a mean of 1 CFU-S per bone marrow sampling unit was estimated to be 17 x 10(6) bone marrow cells, corresponding to a total marrow uptake of approximately 5100 CFU-S (based on a seeding efficiency factor of 10%). If we assume single-hit kinetics, it follows that the recipient W/Wv bone marrow may contain approximately 5100 domains in which stem cell proliferation is geared to the density of the stem cell population. When the various inocula were corrected for multiple seeding in a given domain, the mean inflection point per domain was similar and indicative of five or so divisions before departure from exponential growth at approximately 20% of final CFU-S content 8 days after bone marrow injection. The partitioning of bone marrow into highly localized functional units is consistent with the putative regulatory role of short-range interactions between stem cells and essential stromal elements.

Published

1982

7. In vitro duplication and in vivo cure of mast-cell deficiency of Sl/Sld mutant mice by cloned 3T3 fibroblasts.

Author

Fujita J, Onoue H, Ebi Y, Nakayama H, and Kanakura Y

Subjects

Animals, Cell Differentiation, Cell Division, Cell Line, Cells, Cultured, Fibroblasts transplantation, In Vitro Techniques, Mice, Peritoneal Cavity cytology, Fibroblasts physiology, Mast Cells physiology, Mice, Mutant Strains physiology

Abstract

Sl/Sld mutant mice are profoundly deficient in tissue mast cells as a result of a defect in the microenvironment promoting the development of these cells. To facilitate the analysis of the Sl mutation, we attempted to establish an in vitro system in which the in vivo defect of Sl/Sld mice could be reproduced. 3T3 cell lines were established from 17-day-old embryos of Sl/Sld and congenic +/+ genotypes and were cocultured with mast cells obtained in vitro from the bone marrow of +/+ mice. All eight 3T3 cell lines derived from +/+ of T-cell-derived growth factors. By contrast, none of eight 3T3 cell lines from Sl/Sld embryos supported mast cells under similar conditions. The defect in Sl/Sld 3T3 cells was further characterized as a failure to induce the G1-to-S transition in synchronized mast cells upon contact, suggesting that the Sl gene product is indispensable for this activity. When 3T3 cells of +/+ genotype, grown on pieces of cellulose acetate membrane, were transplanted into the peritoneal cavity of Sl/Sld mice, mast cells appeared locally in the transplanted 3T3 cell layers. These results suggested an essential role of fibroblasts in vivo as the tissue microenvironment promoting the development of mast cells and that they are defective in Sl/Sld mice. The present coculture system duplicated mast-cell deficiency of Sl/Sld mice in vitro and should prove useful for analysis of the Sl gene product.

Published

1989

8. Increased susceptibility to cytomegalovirus infection in beige mutant mice.

Author

Shellam GR, Allan JE, Papadimitriou JM, and Bancroft GJ

Subjects

Animals, Cytomegalovirus Infections immunology, Cytotoxicity, Immunologic, Heterozygote, Homozygote, Immunity, Cellular, Mice, Virus Replication, Cytomegalovirus Infections genetics, Immunity, Innate, Mice, Mutant Strains physiology

Abstract

Mice homozygous for the beige gene (bg/bg) are a homologue of the Chédiak-Higashi syndrome of man and are known to be selectively defective in natural killer (NK) cells. We have compared the susceptibility of bg/bg and bg/+ C57BL/6J mice to infection with murine cytomegalovirus (MCMV). Beige mice are more susceptible to lethal infection and develop 33- to 43-fold higher virus titers in the liver, spleen, and kidney than do bg/+ mice after a sublethal infection, although virus replication is the same in vitro in cultured fibroblasts or epithelial cells from these mice. Inoculation with a sublethal dose of virus stimulates a NK cell response, although this is lower in bg/bg mice despite higher titers of interferon type 1 than in bg/+. A dose of MCMV that is lethal only to bg/bg augments cytotoxicity within 12 hr in bg/+ mice, whereas cytotoxicity in bg/bg remains very low. In bone marrow chimeras, recipients of bg/bg marrow were more susceptible to MCMV and had lower NK cell responses after virus inoculation than did recipients of marrow from bg/+ donors. The greater susceptibility of beige mice to the virus suggests that NK cells may contribute to resistance early in McMV infection.

Published

1981

9. Growth and differentiation of cerebellar suspensions transplanted into the adult cerebellum of mice with heredodegenerative ataxia.

Author

Sotelo C and Alvarado-Mallart RM

Subjects

Animals, Axons ultrastructure, Cell Differentiation, Cell Movement, Cerebellar Ataxia genetics, Cerebellum embryology, Cerebellum pathology, Cerebellum transplantation, Dendrites ultrastructure, Graft Survival, Mice, Mice, Inbred C57BL, Mice, Mutant Strains genetics, Mice, Mutant Strains physiology, Purkinje Cells physiology, Purkinje Cells ultrastructure, Synapses ultrastructure, Cerebellar Ataxia therapy, Purkinje Cells transplantation

Abstract

Cell suspensions from cerebellar primordia of 12-day mouse embryos were grafted into the cerebellum of 4-month-old Purkinje cell degeneration (pcd) mutant mice and examined 2-3 months later. In contrast to those of nontreated mutants, all of the grafted cerebella exhibited Purkinje cells that had migrated into the molecular layer, where they were clustered over its superficial two-thirds. These Purkinje cells develop flattened dendritic trees perpendicular to bundles of parallel fibers. Ultrastructural examination of their synaptic inputs and outputs disclosed that (i) as in normal cerebella, climbing fibers and axons from basket and stellate cells synapse on thick dendrites, whereas parallel fibers almost exclusively contact the distal spiny branchlets, and (ii) a substantial number of Purkinje cell axons reach their appropriate targets in the deep cerebellar nuclei, where they establish synaptic connections on large and small neurons. These results indicate that embryonic Purkinje cells grafted into the cerebellum of adult mice with heredodegenerative ataxia integrate themselves very specifically into the cerebellar circuitry of the recipient mouse, where they can replace the missing Purkinje cells. They also provide a morphological basis favoring the notion of functional restorative capabilities of neural grafts in systems in which neurons are connected in an almost point-to-point manner.

Published

1986