AustralieFrV1, PascalFrancis, Curation, bibRecord, 006D54

Role of medical history in brain tumour development. Results from the international adult brain tumour study

Identifieur interne : 006D54 ( PascalFrancis/Curation ); précédent : 006D53; suivant : 006D55

Role of medical history in brain tumour development. Results from the international adult brain tumour study

Auteurs : B. Schlehofer [Allemagne] ; M. Blettner [Allemagne] ; S. Preston-Martin [États-Unis] ; D. Niehoff [Allemagne] ; J. Wahrendorf [Allemagne] ; A. Arslan [Allemagne] ; A. Ahlbom [Suède] ; W. N. Choi ; G. G. Giles [Australie] ; G. R. Howe [États-Unis] ; J. Little [Royaume-Uni] ; F. Menegoz [France] ; P. Ryan [Australie]

Source :

International journal of cancer [ 0020-7136 ] ; 1999.

RBID : Pascal:99-0375688

Descripteurs français

Pascal (Inist)
- Gliome malin, Intracrânien, Méningiome malin, Antécédent, Association morbide, Epilepsie, Chimiothérapie, Anticonvulsivant, Asthme, Allergie, Eczéma, Etude multicentrique, Etude cas témoin, Homme.
Wicri :
- topic : Allergie, Homme.

English descriptors

KwdEn :
- Allergy, Antecedent, Anticonvulsant, Asthma, Case control study, Chemotherapy, Concomitant disease, Eczema, Epilepsy, Human, Intracranial, Malignant glioma, Malignant meningioma, Multicenter study.

Abstract

In an international population-based case-control study carried out in 8 centres in 6 countries, we investigated the role of specific medical conditions in the aetiology of brain tumours in adults. Recruited were 1,178 glioma and 331 meningioma cases and 2,493 age- and gender-matched population controls. Only medical conditions occurring at least 2 years before brain tumour diagnosis were considered. Relative risks (RRs) and 95% confidence intervals (Cls) were estimated using a conditional logistic regression model. Heterogeneity between centres was tested. No association between meningioma and previous medical conditions was observed. For glioma, there was an increased risk associated with epilepsy (RR = 6.55, 95% Cl 3,40-12.63), but this was considerably weaker for epilepsy of more than 20 years duration. The risk remained elevated after adjustment for use of anti-epileptic drugs. There was a statistically significant inverse association between glioma and all allergic diseases combined (RR = 0.59, 95% Cl 0.49-0.71); this was also observed for specific allergic conditions, namely, asthma and eczema. Subjects who reported a history of infectious diseases (e.g., colds, flu) showed a 30% reduction in risk (RR = 0.72, 95% Cl 0.61-0.85). The decreased risks for glioma in subjects reporting a history of allergic conditions or infectious diseases may indicate an influence of immunological factors on the development of glioma. The association between glioma and epilepsy has to be interpreted cautiously and needs further investigation.

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A11	`02`	`1`		`@1 BLETTNER (M.)`
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A11	`11`	`1`		`@1 LITTLE (J.)`
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A14	`01`			`@1 German Cancer Research Centre, Division of Epidemiology @2 Heidelberg @3 DEU @Z 1 aut. @Z 4 aut. @Z 5 aut.`
A14	`02`			`@1 Department of Epidemiology and Medical Statistics, School of Public Health, University of Bielefeld @2 Bielefeld @3 DEU @Z 2 aut. @Z 6 aut.`
A14	`03`			`@1 University of Southern California School of Medicine @2 Los Angeles, CA @3 USA @Z 3 aut.`
A14	`04`			`@1 Division of Epidemiology, Institute for Environmental Medicine @2 Stockholm @3 SWE @Z 7 aut.`
A14	`05`			`@1 Anti Cancer Council of Victoria @2 Victoria @3 AUS @Z 9 aut.`
A14	`06`			`@1 Division of Epidemiology, Columbia University School of Public Health @2 New York, NY @3 USA @Z 10 aut.`
A14	`07`			`@1 Department of Medicine and Therapeutics, University of Aberdeen Medical School, Foresterhill @2 Aberdeen @3 GBR @Z 11 aut.`
A14	`08`			`@1 Registre du Cancer du Department de l'Isère @2 Meylan @3 FRA @Z 12 aut.`
A14	`09`			`@1 Department of Public Health, University of Adelaide @2 Adelaide @3 AUS @Z 13 aut.`
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C01	`01`		`ENG`	@0 In an international population-based case-control study carried out in 8 centres in 6 countries, we investigated the role of specific medical conditions in the aetiology of brain tumours in adults. Recruited were 1,178 glioma and 331 meningioma cases and 2,493 age- and gender-matched population controls. Only medical conditions occurring at least 2 years before brain tumour diagnosis were considered. Relative risks (RRs) and 95% confidence intervals (Cls) were estimated using a conditional logistic regression model. Heterogeneity between centres was tested. No association between meningioma and previous medical conditions was observed. For glioma, there was an increased risk associated with epilepsy (RR = 6.55, 95% Cl 3,40-12.63), but this was considerably weaker for epilepsy of more than 20 years duration. The risk remained elevated after adjustment for use of anti-epileptic drugs. There was a statistically significant inverse association between glioma and all allergic diseases combined (RR = 0.59, 95% Cl 0.49-0.71); this was also observed for specific allergic conditions, namely, asthma and eczema. Subjects who reported a history of infectious diseases (e.g., colds, flu) showed a 30% reduction in risk (RR = 0.72, 95% Cl 0.61-0.85). The decreased risks for glioma in subjects reporting a history of allergic conditions or infectious diseases may indicate an influence of immunological factors on the development of glioma. The association between glioma and epilepsy has to be interpreted cautiously and needs further investigation.
C02	`01`	`X`		`@0 002B17E`
C03	`01`	`X`	`FRE`	`@0 Gliome malin @5 01`
C03	`01`	`X`	`ENG`	`@0 Malignant glioma @5 01`
C03	`01`	`X`	`SPA`	`@0 Glioma maligno @5 01`
C03	`02`	`X`	`FRE`	`@0 Intracrânien @5 02`
C03	`02`	`X`	`ENG`	`@0 Intracranial @5 02`
C03	`02`	`X`	`SPA`	`@0 Intracraneal @5 02`
C03	`03`	`X`	`FRE`	`@0 Méningiome malin @5 03`
C03	`03`	`X`	`ENG`	`@0 Malignant meningioma @5 03`
C03	`03`	`X`	`SPA`	`@0 Meningioma maligno @5 03`
C03	`04`	`X`	`FRE`	`@0 Antécédent @5 04`
C03	`04`	`X`	`ENG`	`@0 Antecedent @5 04`
C03	`04`	`X`	`SPA`	`@0 Antecedente @5 04`
C03	`05`	`X`	`FRE`	`@0 Association morbide @5 06`
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C03	`05`	`X`	`SPA`	`@0 Asociación morbosa @5 06`
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C03	`07`	`X`	`FRE`	`@0 Chimiothérapie @5 08`
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C03	`07`	`X`	`SPA`	`@0 Quimioterapia @5 08`
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C03	`08`	`X`	`ENG`	`@0 Anticonvulsant @5 09`
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C03	`09`	`X`	`FRE`	`@0 Asthme @5 10`
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C03	`09`	`X`	`SPA`	`@0 Asma @5 10`
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C03	`11`	`X`	`ENG`	`@0 Eczema @5 13`
C03	`11`	`X`	`SPA`	`@0 Eczema @5 13`
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C07	`02`	`X`	`SPA`	`@0 Sistema nervosio central patología @5 38`
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C07	`05`	`X`	`SPA`	`@0 Aparato respiratorio patología @5 61`
C07	`06`	`X`	`FRE`	`@0 Bronchopneumopathie obstructive @5 62`
C07	`06`	`X`	`ENG`	`@0 Obstructive pulmonary disease @5 62`
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C07	`08`	`X`	`FRE`	`@0 Peau pathologie @5 71`
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C07	`08`	`X`	`SPA`	`@0 Piel patología @5 71`
N21				`@1 242`

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<sourceDesc><biblStruct><analytic><title xml:lang="en" level="a">Role of medical history in brain tumour development. Results from the international adult brain tumour study</title>
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<author><name sortKey="Preston Martin, S" sort="Preston Martin, S" uniqKey="Preston Martin S" first="S." last="Preston-Martin">S. Preston-Martin</name>
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<author><name sortKey="Niehoff, D" sort="Niehoff, D" uniqKey="Niehoff D" first="D." last="Niehoff">D. Niehoff</name>
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<s2>Heidelberg</s2>
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<author><name sortKey="Wahrendorf, J" sort="Wahrendorf, J" uniqKey="Wahrendorf J" first="J." last="Wahrendorf">J. Wahrendorf</name>
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<s2>Heidelberg</s2>
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<author><name sortKey="Arslan, A" sort="Arslan, A" uniqKey="Arslan A" first="A." last="Arslan">A. Arslan</name>
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<author><name sortKey="Ahlbom, A" sort="Ahlbom, A" uniqKey="Ahlbom A" first="A." last="Ahlbom">A. Ahlbom</name>
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<s3>SWE</s3>
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<author><name sortKey="Choi, W N" sort="Choi, W N" uniqKey="Choi W" first="W. N." last="Choi">W. N. Choi</name>
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<author><name sortKey="Giles, G G" sort="Giles, G G" uniqKey="Giles G" first="G. G." last="Giles">G. G. Giles</name>
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<author><name sortKey="Howe, G R" sort="Howe, G R" uniqKey="Howe G" first="G. R." last="Howe">G. R. Howe</name>
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<s3>USA</s3>
<sZ>10 aut.</sZ>
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<author><name sortKey="Little, J" sort="Little, J" uniqKey="Little J" first="J." last="Little">J. Little</name>
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<author><name sortKey="Ryan, P" sort="Ryan, P" uniqKey="Ryan P" first="P." last="Ryan">P. Ryan</name>
<affiliation wicri:level="1"><inist:fA14 i1="09"><s1>Department of Public Health, University of Adelaide</s1>
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<series><title level="j" type="main">International journal of cancer</title>
<title level="j" type="abbreviated">Int. j. cancer</title>
<idno type="ISSN">0020-7136</idno>
<imprint><date when="1999">1999</date>
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<seriesStmt><title level="j" type="main">International journal of cancer</title>
<title level="j" type="abbreviated">Int. j. cancer</title>
<idno type="ISSN">0020-7136</idno>
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<profileDesc><textClass><keywords scheme="KwdEn" xml:lang="en"><term>Allergy</term>
<term>Antecedent</term>
<term>Anticonvulsant</term>
<term>Asthma</term>
<term>Case control study</term>
<term>Chemotherapy</term>
<term>Concomitant disease</term>
<term>Eczema</term>
<term>Epilepsy</term>
<term>Human</term>
<term>Intracranial</term>
<term>Malignant glioma</term>
<term>Malignant meningioma</term>
<term>Multicenter study</term>
</keywords>
<keywords scheme="Pascal" xml:lang="fr"><term>Gliome malin</term>
<term>Intracrânien</term>
<term>Méningiome malin</term>
<term>Antécédent</term>
<term>Association morbide</term>
<term>Epilepsie</term>
<term>Chimiothérapie</term>
<term>Anticonvulsivant</term>
<term>Asthme</term>
<term>Allergie</term>
<term>Eczéma</term>
<term>Etude multicentrique</term>
<term>Etude cas témoin</term>
<term>Homme</term>
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<front><div type="abstract" xml:lang="en">In an international population-based case-control study carried out in 8 centres in 6 countries, we investigated the role of specific medical conditions in the aetiology of brain tumours in adults. Recruited were 1,178 glioma and 331 meningioma cases and 2,493 age- and gender-matched population controls. Only medical conditions occurring at least 2 years before brain tumour diagnosis were considered. Relative risks (RRs) and 95% confidence intervals (Cls) were estimated using a conditional logistic regression model. Heterogeneity between centres was tested. No association between meningioma and previous medical conditions was observed. For glioma, there was an increased risk associated with epilepsy (RR = 6.55, 95% Cl 3,40-12.63), but this was considerably weaker for epilepsy of more than 20 years duration. The risk remained elevated after adjustment for use of anti-epileptic drugs. There was a statistically significant inverse association between glioma and all allergic diseases combined (RR = 0.59, 95% Cl 0.49-0.71); this was also observed for specific allergic conditions, namely, asthma and eczema. Subjects who reported a history of infectious diseases (e.g., colds, flu) showed a 30% reduction in risk (RR = 0.72, 95% Cl 0.61-0.85). The decreased risks for glioma in subjects reporting a history of allergic conditions or infectious diseases may indicate an influence of immunological factors on the development of glioma. The association between glioma and epilepsy has to be interpreted cautiously and needs further investigation.</div>
</front>
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<fA08 i1="01" i2="1" l="ENG"><s1>Role of medical history in brain tumour development. Results from the international adult brain tumour study</s1>
</fA08>
<fA11 i1="01" i2="1"><s1>SCHLEHOFER (B.)</s1>
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<fA11 i1="02" i2="1"><s1>BLETTNER (M.)</s1>
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<fA11 i1="03" i2="1"><s1>PRESTON-MARTIN (S.)</s1>
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</fA14>
<fA14 i1="02"><s1>Department of Epidemiology and Medical Statistics, School of Public Health, University of Bielefeld</s1>
<s2>Bielefeld</s2>
<s3>DEU</s3>
<sZ>2 aut.</sZ>
<sZ>6 aut.</sZ>
</fA14>
<fA14 i1="03"><s1>University of Southern California School of Medicine</s1>
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</fA14>
<fA14 i1="04"><s1>Division of Epidemiology, Institute for Environmental Medicine</s1>
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<sZ>7 aut.</sZ>
</fA14>
<fA14 i1="05"><s1>Anti Cancer Council of Victoria</s1>
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<sZ>10 aut.</sZ>
</fA14>
<fA14 i1="07"><s1>Department of Medicine and Therapeutics, University of Aberdeen Medical School, Foresterhill</s1>
<s2>Aberdeen</s2>
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<sZ>11 aut.</sZ>
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<fA14 i1="08"><s1>Registre du Cancer du Department de l'Isère</s1>
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<sZ>12 aut.</sZ>
</fA14>
<fA14 i1="09"><s1>Department of Public Health, University of Adelaide</s1>
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<fC01 i1="01" l="ENG"><s0>In an international population-based case-control study carried out in 8 centres in 6 countries, we investigated the role of specific medical conditions in the aetiology of brain tumours in adults. Recruited were 1,178 glioma and 331 meningioma cases and 2,493 age- and gender-matched population controls. Only medical conditions occurring at least 2 years before brain tumour diagnosis were considered. Relative risks (RRs) and 95% confidence intervals (Cls) were estimated using a conditional logistic regression model. Heterogeneity between centres was tested. No association between meningioma and previous medical conditions was observed. For glioma, there was an increased risk associated with epilepsy (RR = 6.55, 95% Cl 3,40-12.63), but this was considerably weaker for epilepsy of more than 20 years duration. The risk remained elevated after adjustment for use of anti-epileptic drugs. There was a statistically significant inverse association between glioma and all allergic diseases combined (RR = 0.59, 95% Cl 0.49-0.71); this was also observed for specific allergic conditions, namely, asthma and eczema. Subjects who reported a history of infectious diseases (e.g., colds, flu) showed a 30% reduction in risk (RR = 0.72, 95% Cl 0.61-0.85). The decreased risks for glioma in subjects reporting a history of allergic conditions or infectious diseases may indicate an influence of immunological factors on the development of glioma. The association between glioma and epilepsy has to be interpreted cautiously and needs further investigation.</s0>
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<fN21><s1>242</s1>
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Role of medical history in brain tumour development. Results from the international adult brain tumour study

Role of medical history in brain tumour development. Results from the international adult brain tumour study

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