Genetic predisposition to diabetes mellitus is associated with impaired humoral immunity to coxsackievirus B4
Identifieur interne : 00E838 ( Main/Exploration ); précédent : 00E837; suivant : 00E839Genetic predisposition to diabetes mellitus is associated with impaired humoral immunity to coxsackievirus B4
Auteurs : Roger M. Loria [États-Unis] ; Louise B. Montgomery [États-Unis] ; Nancy Tuttle-Fuller [États-Unis] ; Hall M. Gregg [États-Unis] ; Vernon M. Chinchilli [États-Unis]Source :
- Diabetes Research and Clinical Practice [ 0168-8227 ] ; 1986.
Descripteurs français
- Wicri :
- topic : Diabète.
English descriptors
- KwdEn :
- Teeft :
- Average body weight, Blood glucose levels, Body weight, Clinical diabetes, Coat color, Coxsackievirus, Diabetes, Diabetes mellitus, Diabetic, Diabetic gene, Food intake, Genetic background, Genetic predisposition, Glucose, Glucose tolerance test, Heterozygous, Humoral response, Immune competence, Immune response, Inbred, Inbred mice, Infection, Input dose, Libitum, Libitum diet, Libitum food intake, Mellitus, Misty coat color, Misty coat color mice, Mutant, Mutant mice, Mutant mouse, Mutation, Mutation diabetes, Neutralization, Neutralizing antibodies, Overt diabetes, Overt disease, Plaque, Plaque reduction, Same inbred, Serum dilution, Serum dilutions, Single recessive mutation, Virus plaque reduction.
Abstract
Summary: Experiments were performed to determine whether genetic predisposition to diabetes mellitus (DM) or clinical DM or both exert an influence on the production of neutralization antibodies to coxsackievirus B4 (CB4). The homozygous diabetic mutant mouse db+/db+, on the inbred C57BL/KsJ genetic background, develops a diabetes-like disease when maintained on ad libitum diet but rectriction of excess food intake prevents overt disease. The doubly heterozygote db+/+m or the homozygote +m/+m misty coat color mutant, on the C57BL/KsJ genetic background, do not develop DM and served as controls.Animals infected with one-half a previously determined LD50 of CB4 were bled prior to infection and at 3, 5, 7, 14, 21 days and at 1, 2, 3, 4 and 5 months after infection. Serum neutralization antibody (NA) levels were determined from the percent CB4 plaque reduction. Until 2 months following infection, NA levels were not significant in either of the homozygous diabetic mutant groups, db+/db+. In the diabetic mutant group db+/db+, without overt disease, neutralization of CB4 when observed, was low, short-lived, and apparently not specific. However, in the homozygous diabetic mutants with spontaneous diabetes, CB4 NA became evident at 2 months after infection. By 3 months post-infection, serum NA levels were sufficient to cause 90% virus plaque reduction.These observations demonstrate that hereditary DM as characterized by the mutation diabetes, db, in the C57BL/KsJ mouse, is associated with a marked impaired humoral immune response to a diabetogenic human CB4. Specifically, there is an inability to develop an adequate level of anti-CB4 antibodies.The type and degree of immunological impairment are apparently different prior to and after onset of diabetes mellitus.
Url:
DOI: 10.1016/S0168-8227(86)80065-1
Affiliations:
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Loria</name><affiliation wicri:level="2"><country xml:lang="fr">États-Unis</country><wicri:regionArea>Department of Microbiology, School of Basic Sciences, Medical College of Virginia, Virginia Commonwealth University, Richmond, VA</wicri:regionArea><placeName><region type="state">Virginie</region></placeName></affiliation><affiliation wicri:level="2"><country xml:lang="fr" wicri:curation="lc">États-Unis</country><wicri:regionArea>Address all inquiries to: Dr. Roger M. Loria, Department of Microbiology and Immunology, Box 678, Medical College of Virginia, Virginia Commonwealth University, Richmond, VA 23298</wicri:regionArea><placeName><region type="state">Virginie</region></placeName></affiliation><affiliation wicri:level="2"><country xml:lang="fr">États-Unis</country><wicri:regionArea>Department of Microbiology, School of Basic Sciences, Medical College of Virginia, Virginia Commonwealth University, Richmond, VA</wicri:regionArea><placeName><region type="state">Virginie</region></placeName></affiliation></author><author><name sortKey="Montgomery, Louise B" sort="Montgomery, Louise B" uniqKey="Montgomery L" first="Louise B." last="Montgomery">Louise B. 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Gregg</name><affiliation wicri:level="2"><country xml:lang="fr">États-Unis</country><wicri:regionArea>Department of Immunology, School of Basic Sciences, Medical College of Virginia, Virginia Commonwealth University, Richmond, VA</wicri:regionArea><placeName><region type="state">Virginie</region></placeName></affiliation><affiliation wicri:level="2"><country xml:lang="fr">États-Unis</country><wicri:regionArea>Department of Microbiology, School of Basic Sciences, Medical College of Virginia, Virginia Commonwealth University, Richmond, VA</wicri:regionArea><placeName><region type="state">Virginie</region></placeName></affiliation></author><author><name sortKey="Chinchilli, Vernon M" sort="Chinchilli, Vernon M" uniqKey="Chinchilli V" first="Vernon M." last="Chinchilli">Vernon M. Chinchilli</name><affiliation wicri:level="2"><country xml:lang="fr">États-Unis</country><wicri:regionArea>Department of Immunology, School of Basic Sciences, Medical College of Virginia, Virginia Commonwealth University, Richmond, VA</wicri:regionArea><placeName><region type="state">Virginie</region></placeName></affiliation><affiliation wicri:level="2"><country xml:lang="fr">États-Unis</country><wicri:regionArea>Department of Microbiology, School of Basic Sciences, Medical College of Virginia, Virginia Commonwealth University, Richmond, VA</wicri:regionArea><placeName><region type="state">Virginie</region></placeName></affiliation></author></analytic><monogr></monogr><series><title level="j">Diabetes Research and Clinical Practice</title><title level="j" type="abbrev">DIAB</title><idno type="ISSN">0168-8227</idno><imprint><publisher>ELSEVIER</publisher><date type="published" when="1986">1986</date><biblScope unit="volume">2</biblScope><biblScope unit="issue">2</biblScope><biblScope unit="page" from="91">91</biblScope><biblScope unit="page" to="96">96</biblScope></imprint><idno type="ISSN">0168-8227</idno></series></biblStruct></sourceDesc><seriesStmt><idno type="ISSN">0168-8227</idno></seriesStmt></fileDesc><profileDesc><textClass><keywords scheme="KwdEn" xml:lang="en"><term>Coxsackievirus</term><term>Diabetes</term><term>Neutralizing antibodies</term></keywords><keywords scheme="Teeft" xml:lang="en"><term>Average body weight</term><term>Blood glucose levels</term><term>Body weight</term><term>Clinical diabetes</term><term>Coat color</term><term>Coxsackievirus</term><term>Diabetes</term><term>Diabetes mellitus</term><term>Diabetic</term><term>Diabetic gene</term><term>Food intake</term><term>Genetic background</term><term>Genetic predisposition</term><term>Glucose</term><term>Glucose tolerance test</term><term>Heterozygous</term><term>Humoral response</term><term>Immune competence</term><term>Immune response</term><term>Inbred</term><term>Inbred mice</term><term>Infection</term><term>Input dose</term><term>Libitum</term><term>Libitum diet</term><term>Libitum food intake</term><term>Mellitus</term><term>Misty coat color</term><term>Misty coat color mice</term><term>Mutant</term><term>Mutant mice</term><term>Mutant mouse</term><term>Mutation</term><term>Mutation diabetes</term><term>Neutralization</term><term>Neutralizing antibodies</term><term>Overt diabetes</term><term>Overt disease</term><term>Plaque</term><term>Plaque reduction</term><term>Same inbred</term><term>Serum dilution</term><term>Serum dilutions</term><term>Single recessive mutation</term><term>Virus plaque reduction</term></keywords><keywords scheme="Wicri" type="topic" xml:lang="fr"><term>Diabète</term></keywords></textClass><langUsage><language ident="en">en</language></langUsage></profileDesc></teiHeader><front><div type="abstract" xml:lang="en">Summary: Experiments were performed to determine whether genetic predisposition to diabetes mellitus (DM) or clinical DM or both exert an influence on the production of neutralization antibodies to coxsackievirus B4 (CB4). The homozygous diabetic mutant mouse db+/db+, on the inbred C57BL/KsJ genetic background, develops a diabetes-like disease when maintained on ad libitum diet but rectriction of excess food intake prevents overt disease. The doubly heterozygote db+/+m or the homozygote +m/+m misty coat color mutant, on the C57BL/KsJ genetic background, do not develop DM and served as controls.Animals infected with one-half a previously determined LD50 of CB4 were bled prior to infection and at 3, 5, 7, 14, 21 days and at 1, 2, 3, 4 and 5 months after infection. Serum neutralization antibody (NA) levels were determined from the percent CB4 plaque reduction. Until 2 months following infection, NA levels were not significant in either of the homozygous diabetic mutant groups, db+/db+. In the diabetic mutant group db+/db+, without overt disease, neutralization of CB4 when observed, was low, short-lived, and apparently not specific. However, in the homozygous diabetic mutants with spontaneous diabetes, CB4 NA became evident at 2 months after infection. By 3 months post-infection, serum NA levels were sufficient to cause 90% virus plaque reduction.These observations demonstrate that hereditary DM as characterized by the mutation diabetes, db, in the C57BL/KsJ mouse, is associated with a marked impaired humoral immune response to a diabetogenic human CB4. Specifically, there is an inability to develop an adequate level of anti-CB4 antibodies.The type and degree of immunological impairment are apparently different prior to and after onset of diabetes mellitus.</div></front></TEI><affiliations><list><country><li>États-Unis</li></country><region><li>Virginie</li></region></list><tree><country name="États-Unis"><region name="Virginie"><name sortKey="Loria, Roger M" sort="Loria, Roger M" uniqKey="Loria R" first="Roger M." last="Loria">Roger M. Loria</name></region><name sortKey="Chinchilli, Vernon M" sort="Chinchilli, Vernon M" uniqKey="Chinchilli V" first="Vernon M." last="Chinchilli">Vernon M. Chinchilli</name><name sortKey="Chinchilli, Vernon M" sort="Chinchilli, Vernon M" uniqKey="Chinchilli V" first="Vernon M." last="Chinchilli">Vernon M. Chinchilli</name><name sortKey="Gregg, Hall M" sort="Gregg, Hall M" uniqKey="Gregg H" first="Hall M." last="Gregg">Hall M. Gregg</name><name sortKey="Gregg, Hall M" sort="Gregg, Hall M" uniqKey="Gregg H" first="Hall M." last="Gregg">Hall M. Gregg</name><name sortKey="Loria, Roger M" sort="Loria, Roger M" uniqKey="Loria R" first="Roger M." last="Loria">Roger M. Loria</name><name sortKey="Loria, Roger M" sort="Loria, Roger M" uniqKey="Loria R" first="Roger M." last="Loria">Roger M. Loria</name><name sortKey="Montgomery, Louise B" sort="Montgomery, Louise B" uniqKey="Montgomery L" first="Louise B." last="Montgomery">Louise B. Montgomery</name><name sortKey="Montgomery, Louise B" sort="Montgomery, Louise B" uniqKey="Montgomery L" first="Louise B." last="Montgomery">Louise B. Montgomery</name><name sortKey="Tuttle Fuller, Nancy" sort="Tuttle Fuller, Nancy" uniqKey="Tuttle Fuller N" first="Nancy" last="Tuttle-Fuller">Nancy Tuttle-Fuller</name><name sortKey="Tuttle Fuller, Nancy" sort="Tuttle Fuller, Nancy" uniqKey="Tuttle Fuller N" first="Nancy" last="Tuttle-Fuller">Nancy Tuttle-Fuller</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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