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Granulomatous disease in CVID: retrospective analysis of clinical characteristics and treatment efficacy in a cohort of 59 patients.

Identifieur interne : 000106 ( Hal/Corpus ); précédent : 000105; suivant : 000107

Granulomatous disease in CVID: retrospective analysis of clinical characteristics and treatment efficacy in a cohort of 59 patients.

Auteurs : Jean-Nicolas Boursiquot ; Laurence Gérard ; Marion Malphettes ; Claire Fieschi ; Lionel Galicier ; David Boutboul ; Raphael Borie ; Jean-François Viallard ; Pauline Soulas-Sprauel ; Alice Berezne ; Arnaud Jaccard ; Eric Hachulla ; Julien Haroche ; Nicolas Schleinitz ; Laurent Têtu ; Eric Oksenhendler ; Non Renseigné

Source :

RBID : Hal:hal-00945425

Abstract

BACKGROUND: Granulomatous disease (GD) will develop in a subset of patients with common variable immunodeficiency (CVID). Little is known about the efficacy of therapeutic agents used for treating this disorder. OBJECTIVE: To evaluate the efficacy of immunosuppressive drugs with the help of a set of clinical, biological and radiological criteria. METHOD: Clinical and laboratory features of CVID patients were collected from the French DEFI cohort, a prospective study on adults with hypogammaglobulinemia. The medical charts of 55 patients (93 %) of the GD cohort were reviewed. RESULTS: Among 436 subjects with CVID, 59 patients (13.5 %) were diagnosed with GD. Of the 55 patients in whom medical charts were available, 32 patients received treatment for the granulomatous disease. Corticosteroids were the most frequently used drug. Complete response to treatment was infrequent. It was achieved with corticosteroids, cyclophosphamide, hydroxychloroquine, rituximab and methotrexate. Azathioprine, cyclosporine, mycophenolate mofetil, sirolimus, infliximab and thalidomide led to partial or absence of response. Complete and partial responses were observed in lymph nodes, lungs, liver, skin, bone marrow and central nervous system. Absent of response for gastrointestinal tract granulomas was noted in all cases of treatment attempt. CONCLUSION: CVID patients with GD exhibit a particular biological phenotype. Treatment should be considered in any symptomatic patient or if there is evidence of organ dysfunction. Corticosteroids are the drug of choice in most instances but response to treatment is often unsatisfactory.


Url:
DOI: 10.1007/s10875-012-9778-9

Links to Exploration step

Hal:hal-00945425

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<p>BACKGROUND: Granulomatous disease (GD) will develop in a subset of patients with common variable immunodeficiency (CVID). Little is known about the efficacy of therapeutic agents used for treating this disorder. OBJECTIVE: To evaluate the efficacy of immunosuppressive drugs with the help of a set of clinical, biological and radiological criteria. METHOD: Clinical and laboratory features of CVID patients were collected from the French DEFI cohort, a prospective study on adults with hypogammaglobulinemia. The medical charts of 55 patients (93 %) of the GD cohort were reviewed. RESULTS: Among 436 subjects with CVID, 59 patients (13.5 %) were diagnosed with GD. Of the 55 patients in whom medical charts were available, 32 patients received treatment for the granulomatous disease. Corticosteroids were the most frequently used drug. Complete response to treatment was infrequent. It was achieved with corticosteroids, cyclophosphamide, hydroxychloroquine, rituximab and methotrexate. Azathioprine, cyclosporine, mycophenolate mofetil, sirolimus, infliximab and thalidomide led to partial or absence of response. Complete and partial responses were observed in lymph nodes, lungs, liver, skin, bone marrow and central nervous system. Absent of response for gastrointestinal tract granulomas was noted in all cases of treatment attempt. CONCLUSION: CVID patients with GD exhibit a particular biological phenotype. Treatment should be considered in any symptomatic patient or if there is evidence of organ dysfunction. Corticosteroids are the drug of choice in most instances but response to treatment is often unsatisfactory.</p>
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<forename type="first">Claire</forename>
<surname>Fieschi</surname>
</persName>
<idno type="halauthorid">196216</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Lionel</forename>
<surname>Galicier</surname>
</persName>
<idno type="halauthorid">464500</idno>
</author>
<author role="aut">
<persName>
<forename type="first">David</forename>
<surname>Boutboul</surname>
</persName>
<idno type="halauthorid">743930</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Raphael</forename>
<surname>Borie</surname>
</persName>
<idno type="halauthorid">983685</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Jean-François</forename>
<surname>Viallard</surname>
</persName>
<idno type="halauthorid">81314</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Pauline</forename>
<surname>Soulas-Sprauel</surname>
</persName>
<idno type="halauthorid">202980</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Alice</forename>
<surname>Berezne</surname>
</persName>
<idno type="halauthorid">846751</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Arnaud</forename>
<surname>Jaccard</surname>
</persName>
<email type="md5">810e17e57ec412f1f2003c1386328fb5</email>
<email type="domain">unilim.fr</email>
<idno type="halauthorid">1242269</idno>
<affiliation ref="#struct-827"></affiliation>
<affiliation ref="#struct-70800"></affiliation>
</author>
<author role="aut">
<persName>
<forename type="first">Eric</forename>
<surname>Hachulla</surname>
</persName>
<idno type="halauthorid">238132</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Julien</forename>
<surname>Haroche</surname>
</persName>
<idno type="halauthorid">648404</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Nicolas</forename>
<surname>Schleinitz</surname>
</persName>
<idno type="halauthorid">464501</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Laurent</forename>
<surname>Têtu</surname>
</persName>
<idno type="halauthorid">983686</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Eric</forename>
<surname>Oksenhendler</surname>
</persName>
<idno type="halauthorid">451301</idno>
</author>
<author role="aut">
<persName>
<forename type="first">Non</forename>
<surname>Renseigné</surname>
</persName>
<idno type="halauthorid">343490</idno>
</author>
</analytic>
<monogr>
<idno type="halJournalId" status="VALID">15227</idno>
<idno type="issn">0271-9142</idno>
<idno type="eissn">1573-2592</idno>
<title level="j">Journal of Clinical Immunology</title>
<imprint>
<publisher>Springer Verlag</publisher>
<biblScope unit="volume">33</biblScope>
<biblScope unit="issue">1</biblScope>
<biblScope unit="pp">84-95</biblScope>
<date type="datePub">2013-01</date>
<date type="dateEpub">2012-09-18</date>
</imprint>
</monogr>
<idno type="doi">10.1007/s10875-012-9778-9</idno>
<idno type="pubmed">22986767</idno>
</biblStruct>
</sourceDesc>
<profileDesc>
<langUsage>
<language ident="en">English</language>
</langUsage>
<textClass>
<classCode scheme="mesh">Adult</classCode>
<classCode scheme="mesh">Agammaglobulinemia</classCode>
<classCode scheme="mesh">Infant</classCode>
<classCode scheme="mesh">Infant, Newborn</classCode>
<classCode scheme="mesh">Male</classCode>
<classCode scheme="mesh">Organ Specificity</classCode>
<classCode scheme="mesh">Prospective Studies</classCode>
<classCode scheme="mesh">Retrospective Studies</classCode>
<classCode scheme="mesh">Treatment Outcome</classCode>
<classCode scheme="mesh">Child</classCode>
<classCode scheme="mesh">Child, Preschool</classCode>
<classCode scheme="mesh">Cohort Studies</classCode>
<classCode scheme="mesh">Common Variable Immunodeficiency</classCode>
<classCode scheme="mesh">Female</classCode>
<classCode scheme="mesh">Granulomatous Disease, Chronic</classCode>
<classCode scheme="mesh">Humans</classCode>
<classCode scheme="mesh">Immunophenotyping</classCode>
<classCode scheme="halDomain" n="sdv.imm">Life Sciences [q-bio]/Immunology</classCode>
<classCode scheme="halTypology" n="ART">Journal articles</classCode>
</textClass>
<abstract xml:lang="en">
<p>BACKGROUND: Granulomatous disease (GD) will develop in a subset of patients with common variable immunodeficiency (CVID). Little is known about the efficacy of therapeutic agents used for treating this disorder. OBJECTIVE: To evaluate the efficacy of immunosuppressive drugs with the help of a set of clinical, biological and radiological criteria. METHOD: Clinical and laboratory features of CVID patients were collected from the French DEFI cohort, a prospective study on adults with hypogammaglobulinemia. The medical charts of 55 patients (93 %) of the GD cohort were reviewed. RESULTS: Among 436 subjects with CVID, 59 patients (13.5 %) were diagnosed with GD. Of the 55 patients in whom medical charts were available, 32 patients received treatment for the granulomatous disease. Corticosteroids were the most frequently used drug. Complete response to treatment was infrequent. It was achieved with corticosteroids, cyclophosphamide, hydroxychloroquine, rituximab and methotrexate. Azathioprine, cyclosporine, mycophenolate mofetil, sirolimus, infliximab and thalidomide led to partial or absence of response. Complete and partial responses were observed in lymph nodes, lungs, liver, skin, bone marrow and central nervous system. Absent of response for gastrointestinal tract granulomas was noted in all cases of treatment attempt. CONCLUSION: CVID patients with GD exhibit a particular biological phenotype. Treatment should be considered in any symptomatic patient or if there is evidence of organ dysfunction. Corticosteroids are the drug of choice in most instances but response to treatment is often unsatisfactory.</p>
</abstract>
</profileDesc>
</hal>
</record>

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