The utility of fine needle aspiration in HIV positive children
Identifieur interne : 001C63 ( Istex/Corpus ); précédent : 001C62; suivant : 001C64The utility of fine needle aspiration in HIV positive children
Auteurs : P. Michelow ; T. Meyers ; M. Dubb ; C. WrightSource :
- Cytopathology [ 0956-5507 ] ; 2008-04.
English descriptors
- KwdEn :
- Abdominal masses, Acta cytol, African department, Anatomical pathology, Ancillary studies form, Antiretroviral therapy, Aspirate, Aspirate mass lesions, Aspiration, Axillary masses groin masses, Biopsy, Blackwell publishing, Buttock masses, Cell borders, Chest wall mass, Cohesive spindle cells, Common presentation, Current study, Cytological, Cytological diagnosis, Cytology, Cytology unit, Cytometry, Cytopathology, Cytoplasmic ratio, Diagn cytopathol, Dual population, Eosinophilic cytoplasm, Epithelial cells, Epithelioid histiocytes, Fine needle aspiration, Fine needle aspiration biopsy, Fine needle aspiration cytology, Flow cytometry, Fnas, Fungal infection, Granular chromatin, Haemorrhagic background, Hivinfected children, Human virus, Immature lymphocytes, Inadequate fnas, Kaposi, Kaposi sarcoma, Larger cells, Lesion, Long arrow, Lung mass, Lymph nodes, Lymphadenopathy, Lymphadenpathy, Lymphoepithelial lesion, Lymphoid cells, Lymphoma, Many children, Mass lesion, Mass lesions, Melanotic progonoma, Minimal amounts, Monomorphic population, Mycobacterial, Mycobacterial infection, National health laboratory service, National health laboratory service journal compilation, Neck masses, Needle aspirates, Needle aspiration, Needle aspiration cytology, Numerous yeasts, Occasional cells, Occasional groups, Papanicolaou stain, Positive adults, Positive children, Pregnant women, Rapid diagnosis obviating, Reactive, Reactive lymphadenopathy, Reactive lymphadenpathy, Recurrent lymphoma, Rhabdomyosarcoma, Salivary gland swellings, Sarcoma, Several studies, Small blastemal cells, Smooth muscle tumours, Spindle cells, Swift treatment, Syphilis prevalence survey, Tingible body macrophages, Universal safety precautions, Worthwhile procedure.
- Teeft :
- Abdominal masses, Acta cytol, African department, Anatomical pathology, Ancillary studies form, Antiretroviral therapy, Aspirate, Aspirate mass lesions, Aspiration, Axillary masses groin masses, Biopsy, Blackwell publishing, Buttock masses, Cell borders, Chest wall mass, Cohesive spindle cells, Common presentation, Current study, Cytological, Cytological diagnosis, Cytology, Cytology unit, Cytometry, Cytopathology, Cytoplasmic ratio, Diagn cytopathol, Dual population, Eosinophilic cytoplasm, Epithelial cells, Epithelioid histiocytes, Fine needle aspiration, Fine needle aspiration biopsy, Fine needle aspiration cytology, Flow cytometry, Fnas, Fungal infection, Granular chromatin, Haemorrhagic background, Hivinfected children, Human virus, Immature lymphocytes, Inadequate fnas, Kaposi, Kaposi sarcoma, Larger cells, Lesion, Long arrow, Lung mass, Lymph nodes, Lymphadenopathy, Lymphadenpathy, Lymphoepithelial lesion, Lymphoid cells, Lymphoma, Many children, Mass lesion, Mass lesions, Melanotic progonoma, Minimal amounts, Monomorphic population, Mycobacterial, Mycobacterial infection, National health laboratory service, National health laboratory service journal compilation, Neck masses, Needle aspirates, Needle aspiration, Needle aspiration cytology, Numerous yeasts, Occasional cells, Occasional groups, Papanicolaou stain, Positive adults, Positive children, Pregnant women, Rapid diagnosis obviating, Reactive, Reactive lymphadenopathy, Reactive lymphadenpathy, Recurrent lymphoma, Rhabdomyosarcoma, Salivary gland swellings, Sarcoma, Several studies, Small blastemal cells, Smooth muscle tumours, Spindle cells, Swift treatment, Syphilis prevalence survey, Tingible body macrophages, Universal safety precautions, Worthwhile procedure.
Abstract
Objective: To determine the spectrum of disease, diagnostic accuracy and adequacy of fine needle aspirates (FNA) in human immunodeficiency virus (HIV) positive children who present with mass lesions.
Url:
DOI: 10.1111/j.1365-2303.2007.00474.x
Links to Exploration step
ISTEX:57FD5B2DC4DD2C47C242710C928FB67C60BF420BLe document en format XML
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Michelow</name><affiliation><mods:affiliation>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa</mods:affiliation></affiliation></author><author><name sortKey="Meyers, T" sort="Meyers, T" uniqKey="Meyers T" first="T." last="Meyers">T. Meyers</name><affiliation><mods:affiliation>Harriet Shezi Children’s Clinic, Department of Paediatrics, Chris Hani Baragwanath Hospital, and University of the Witwatersrand, Johannesburg, South Africa</mods:affiliation></affiliation></author><author><name sortKey="Dubb, M" sort="Dubb, M" uniqKey="Dubb M" first="M." last="Dubb">M. Dubb</name><affiliation><mods:affiliation>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa</mods:affiliation></affiliation></author><author><name sortKey="Wright, C" sort="Wright, C" uniqKey="Wright C" first="C." last="Wright">C. 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xml:lang="en"><term>Abdominal masses</term><term>Acta cytol</term><term>African department</term><term>Anatomical pathology</term><term>Ancillary studies form</term><term>Antiretroviral therapy</term><term>Aspirate</term><term>Aspirate mass lesions</term><term>Aspiration</term><term>Axillary masses groin masses</term><term>Biopsy</term><term>Blackwell publishing</term><term>Buttock masses</term><term>Cell borders</term><term>Chest wall mass</term><term>Cohesive spindle cells</term><term>Common presentation</term><term>Current study</term><term>Cytological</term><term>Cytological diagnosis</term><term>Cytology</term><term>Cytology unit</term><term>Cytometry</term><term>Cytopathology</term><term>Cytoplasmic ratio</term><term>Diagn cytopathol</term><term>Dual population</term><term>Eosinophilic cytoplasm</term><term>Epithelial cells</term><term>Epithelioid histiocytes</term><term>Fine needle aspiration</term><term>Fine needle aspiration biopsy</term><term>Fine needle aspiration cytology</term><term>Flow cytometry</term><term>Fnas</term><term>Fungal infection</term><term>Granular chromatin</term><term>Haemorrhagic background</term><term>Hivinfected children</term><term>Human virus</term><term>Immature lymphocytes</term><term>Inadequate fnas</term><term>Kaposi</term><term>Kaposi sarcoma</term><term>Larger cells</term><term>Lesion</term><term>Long arrow</term><term>Lung mass</term><term>Lymph nodes</term><term>Lymphadenopathy</term><term>Lymphadenpathy</term><term>Lymphoepithelial lesion</term><term>Lymphoid cells</term><term>Lymphoma</term><term>Many children</term><term>Mass lesion</term><term>Mass lesions</term><term>Melanotic progonoma</term><term>Minimal amounts</term><term>Monomorphic population</term><term>Mycobacterial</term><term>Mycobacterial infection</term><term>National health laboratory service</term><term>National health laboratory service journal compilation</term><term>Neck masses</term><term>Needle aspirates</term><term>Needle aspiration</term><term>Needle aspiration cytology</term><term>Numerous yeasts</term><term>Occasional cells</term><term>Occasional groups</term><term>Papanicolaou stain</term><term>Positive adults</term><term>Positive children</term><term>Pregnant women</term><term>Rapid diagnosis obviating</term><term>Reactive</term><term>Reactive lymphadenopathy</term><term>Reactive lymphadenpathy</term><term>Recurrent lymphoma</term><term>Rhabdomyosarcoma</term><term>Salivary gland swellings</term><term>Sarcoma</term><term>Several studies</term><term>Small blastemal cells</term><term>Smooth muscle tumours</term><term>Spindle cells</term><term>Swift treatment</term><term>Syphilis prevalence survey</term><term>Tingible body macrophages</term><term>Universal safety precautions</term><term>Worthwhile procedure</term></keywords><keywords scheme="Teeft" xml:lang="en"><term>Abdominal masses</term><term>Acta cytol</term><term>African department</term><term>Anatomical pathology</term><term>Ancillary studies form</term><term>Antiretroviral therapy</term><term>Aspirate</term><term>Aspirate mass lesions</term><term>Aspiration</term><term>Axillary masses groin masses</term><term>Biopsy</term><term>Blackwell publishing</term><term>Buttock masses</term><term>Cell borders</term><term>Chest wall mass</term><term>Cohesive spindle cells</term><term>Common presentation</term><term>Current study</term><term>Cytological</term><term>Cytological diagnosis</term><term>Cytology</term><term>Cytology unit</term><term>Cytometry</term><term>Cytopathology</term><term>Cytoplasmic ratio</term><term>Diagn cytopathol</term><term>Dual population</term><term>Eosinophilic cytoplasm</term><term>Epithelial cells</term><term>Epithelioid histiocytes</term><term>Fine needle aspiration</term><term>Fine needle aspiration biopsy</term><term>Fine needle aspiration cytology</term><term>Flow cytometry</term><term>Fnas</term><term>Fungal infection</term><term>Granular chromatin</term><term>Haemorrhagic background</term><term>Hivinfected children</term><term>Human virus</term><term>Immature lymphocytes</term><term>Inadequate fnas</term><term>Kaposi</term><term>Kaposi sarcoma</term><term>Larger cells</term><term>Lesion</term><term>Long arrow</term><term>Lung mass</term><term>Lymph nodes</term><term>Lymphadenopathy</term><term>Lymphadenpathy</term><term>Lymphoepithelial lesion</term><term>Lymphoid cells</term><term>Lymphoma</term><term>Many children</term><term>Mass lesion</term><term>Mass lesions</term><term>Melanotic progonoma</term><term>Minimal amounts</term><term>Monomorphic population</term><term>Mycobacterial</term><term>Mycobacterial infection</term><term>National health laboratory service</term><term>National health laboratory service journal compilation</term><term>Neck masses</term><term>Needle aspirates</term><term>Needle aspiration</term><term>Needle aspiration cytology</term><term>Numerous yeasts</term><term>Occasional cells</term><term>Occasional groups</term><term>Papanicolaou stain</term><term>Positive adults</term><term>Positive children</term><term>Pregnant women</term><term>Rapid diagnosis obviating</term><term>Reactive</term><term>Reactive lymphadenopathy</term><term>Reactive lymphadenpathy</term><term>Recurrent lymphoma</term><term>Rhabdomyosarcoma</term><term>Salivary gland swellings</term><term>Sarcoma</term><term>Several studies</term><term>Small blastemal cells</term><term>Smooth muscle tumours</term><term>Spindle cells</term><term>Swift treatment</term><term>Syphilis prevalence survey</term><term>Tingible body macrophages</term><term>Universal safety precautions</term><term>Worthwhile procedure</term></keywords></textClass></profileDesc></teiHeader><front><div type="abstract">Objective: To determine the spectrum of disease, diagnostic accuracy and adequacy of fine needle aspirates (FNA) in human immunodeficiency virus (HIV) positive children who present with mass 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Michelow</name><affiliations><json:string>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa</json:string></affiliations></json:item><json:item><name>T. Meyers</name><affiliations><json:string>Harriet Shezi Children’s Clinic, Department of Paediatrics, Chris Hani Baragwanath Hospital, and University of the Witwatersrand, Johannesburg, South Africa</json:string></affiliations></json:item><json:item><name>M. Dubb</name><affiliations><json:string>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa</json:string></affiliations></json:item><json:item><name>C. Wright</name><affiliations><json:string>Department of Anatomical Pathology, Tygerberg hospital, National Health Laboratory Service, University of Stellenbosch, Cape Town, South Africa</json:string></affiliations></json:item></author><subject><json:item><lang><json:string>eng</json:string></lang><value>fine needle aspirates</value></json:item><json:item><lang><json:string>eng</json:string></lang><value>human immunodeficiency virus</value></json:item><json:item><lang><json:string>eng</json:string></lang><value>paediatric population</value></json:item><json:item><lang><json:string>eng</json:string></lang><value>reactive lymphadenopathy</value></json:item><json:item><lang><json:string>eng</json:string></lang><value>mycobacterial infection</value></json:item><json:item><lang><json:string>eng</json:string></lang><value>cytodiagnosis</value></json:item><json:item><lang><json:string>eng</json:string></lang><value>cytological technique</value></json:item><json:item><lang><json:string>eng</json:string></lang><value>laboratory diagnosis</value></json:item></subject><articleId><json:string>CYT474</json:string></articleId><language><json:string>eng</json:string></language><originalGenre><json:string>article</json:string></originalGenre><qualityIndicators><score>4.167</score><pdfVersion>1.3</pdfVersion><pdfPageSize>595.276 x 782.362 pts</pdfPageSize><refBibsNative>true</refBibsNative><abstractCharCount>200</abstractCharCount><pdfWordCount>3831</pdfWordCount><pdfCharCount>25772</pdfCharCount><pdfPageCount>8</pdfPageCount><abstractWordCount>28</abstractWordCount></qualityIndicators><title>The utility of fine needle aspiration in HIV positive 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children</title></titleStmt><publicationStmt><authority>ISTEX</authority><publisher>Blackwell Publishing Ltd</publisher><pubPlace>Oxford, UK</pubPlace><availability><licence>© 2007 National Health Laboratory Service</licence></availability><date type="published" when="2008-04"></date></publicationStmt><notesStmt><note type="content-type" subtype="article" source="article" scheme="https://content-type.data.istex.fr/ark:/67375/XTP-6N5SZHKN-D">article</note><note type="publication-type" subtype="journal" scheme="https://publication-type.data.istex.fr/ark:/67375/JMC-0GLKJH51-B">journal</note></notesStmt><sourceDesc><biblStruct type="article"><analytic><title level="a" type="main">The utility of fine needle aspiration in HIV positive children</title><title level="a" type="short">Utility of fine needle aspiration in HIV positive children</title><author xml:id="author-0000"><persName><forename type="first">P.</forename><surname>Michelow</surname></persName><affiliation>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa<address><country key="ZA"></country></address></affiliation></author><author xml:id="author-0001"><persName><forename type="first">T.</forename><surname>Meyers</surname></persName><affiliation>Harriet Shezi Children’s Clinic, Department of Paediatrics, Chris Hani Baragwanath Hospital, and University of the Witwatersrand, Johannesburg, South Africa<address><country key="ZA"></country></address></affiliation></author><author xml:id="author-0002"><persName><forename type="first">M.</forename><surname>Dubb</surname></persName><affiliation>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa<address><country key="ZA"></country></address></affiliation></author><author xml:id="author-0003"><persName><forename type="first">C.</forename><surname>Wright</surname></persName><affiliation>Department of Anatomical Pathology, Tygerberg hospital, National Health Laboratory Service, University of Stellenbosch, Cape Town, South Africa<address><country key="ZA"></country></address></affiliation></author><idno type="istex">57FD5B2DC4DD2C47C242710C928FB67C60BF420B</idno><idno type="ark">ark:/67375/WNG-0N94MRFR-T</idno><idno type="DOI">10.1111/j.1365-2303.2007.00474.x</idno><idno type="unit">CYT474</idno><idno type="toTypesetVersion">file:CYT.CYT474.pdf</idno></analytic><monogr><title level="j" type="main">Cytopathology</title><title level="j" type="alt">CYTOPATHOLOGY</title><idno type="pISSN">0956-5507</idno><idno type="eISSN">1365-2303</idno><idno type="book-DOI">10.1111/(ISSN)1365-2303</idno><idno type="book-part-DOI">10.1111/cyt.2008.19.issue-2</idno><idno type="product">CYT</idno><idno type="publisherDivision">ST</idno><imprint><biblScope unit="vol">19</biblScope><biblScope unit="issue">2</biblScope><biblScope unit="page" from="86">86</biblScope><biblScope unit="page" to="93">93</biblScope><biblScope unit="page-count">8</biblScope><publisher>Blackwell Publishing Ltd</publisher><pubPlace>Oxford, UK</pubPlace><date type="published" when="2008-04"></date></imprint></monogr></biblStruct></sourceDesc></fileDesc><profileDesc><abstract xml:lang="en" style="main"><p><hi rend="bold">Objective: </hi> To determine the spectrum of disease, diagnostic accuracy and adequacy of fine needle aspirates (FNA) in human immunodeficiency virus (HIV) positive children who present with mass lesions.</p><p><hi rend="bold">Methods: </hi> Between January 1997 and December 2002, 95 FNAs were performed in 91 children aged 15 years and younger who were known to be infected with the human immunodeficiency virus (HIV).</p><p><hi rend="bold">Results: </hi> Head and neck masses including salivary gland swellings were the most common presentation (58.9%) followed by axillary masses (25.3%). Groin masses were aspirated in six children, flank and abdominal masses in four children, buttock masses in three children, a chest wall mass in one child and a sonar guided FNA of a lung mass in one child. Eight FNAs (8.4%) proved inadequate. Reactive lymphadenopathy was diagnosed in 42 cases, mycobacterial infection in 22, four children were diagnosed with abscess, one child had a fungal infection and five were found to have non‐Hodgkin’s lymphoma. There were four cases each of lymphoepithelial lesion and Kaposi sarcoma. There was one case each of nephroblastoma, rhabdomyosarcoma, myeloma, melanotic progonoma and spindle cells, not otherwise specified.</p><p><hi rend="bold">Conclusion: </hi> Fine needle aspiration in HIV positive children is a worthwhile procedure and in most instances allows a rapid diagnosis obviating the need for surgery and enabling swift treatment to be undertaken where necessary. Ancillary studies form an important diagnostic component. Universal safety precautions must be strictly adhered to.</p></abstract><textClass><keywords xml:lang="en"><term xml:id="k1">fine needle aspirates</term><term xml:id="k2">human immunodeficiency virus</term><term xml:id="k3">paediatric population</term><term xml:id="k4">reactive lymphadenopathy</term><term xml:id="k5">mycobacterial infection</term><term xml:id="k6">cytodiagnosis</term><term xml:id="k7">cytological technique</term><term xml:id="k8">laboratory diagnosis</term></keywords><keywords rend="tocHeading1"><term>Original articles</term></keywords></textClass><langUsage><language ident="en"></language></langUsage></profileDesc></teiHeader></istex:fulltextTEI><json:item><extension>txt</extension><original>false</original><mimetype>text/plain</mimetype><uri>https://api.istex.fr/document/57FD5B2DC4DD2C47C242710C928FB67C60BF420B/fulltext/txt</uri></json:item></fulltext><metadata><istex:metadataXml wicri:clean="Wiley, elements deleted: body"><istex:xmlDeclaration>version="1.0" encoding="UTF-8" standalone="yes"</istex:xmlDeclaration><istex:document><component version="2.0" type="serialArticle" xml:lang="en"><header><publicationMeta level="product"><publisherInfo><publisherName>Blackwell Publishing Ltd</publisherName><publisherLoc>Oxford, UK</publisherLoc></publisherInfo><doi origin="wiley" registered="yes">10.1111/(ISSN)1365-2303</doi><issn type="print">0956-5507</issn><issn type="electronic">1365-2303</issn><idGroup><id type="product" value="CYT"></id><id type="publisherDivision" value="ST"></id></idGroup><titleGroup><title type="main" sort="CYTOPATHOLOGY">Cytopathology</title></titleGroup></publicationMeta><publicationMeta level="part" position="04002"><doi origin="wiley">10.1111/cyt.2008.19.issue-2</doi><numberingGroup><numbering type="journalVolume" number="19">19</numbering><numbering type="journalIssue" number="2">2</numbering></numberingGroup><coverDate startDate="2008-04">April 2008</coverDate></publicationMeta><publicationMeta level="unit" type="article" position="4" status="forIssue"><doi origin="wiley">10.1111/j.1365-2303.2007.00474.x</doi><idGroup><id type="unit" value="CYT474"></id></idGroup><countGroup><count type="pageTotal" number="8"></count></countGroup><titleGroup><title type="tocHeading1">Original articles</title></titleGroup><copyright>© 2007 National Health Laboratory Service</copyright><eventGroup><event type="firstOnline" date="2007-10-04"></event><event type="publishedOnlineFinalForm" date="2007-10-04"></event><event type="xmlConverted" agent="Converter:BPG_TO_WML3G version:2.3.2 mode:FullText source:FullText result:FullText" date="2010-03-16"></event><event type="xmlConverted" agent="Converter:WILEY_ML3G_TO_WILEY_ML3GV2 version:3.8.8" date="2014-01-16"></event><event type="xmlConverted" agent="Converter:WML3G_To_WML3G version:4.1.7 mode:FullText,remove_FC" date="2014-10-16"></event></eventGroup><numberingGroup><numbering type="pageFirst" number="86">86</numbering><numbering type="pageLast" number="93">93</numbering></numberingGroup><correspondenceTo>Dr P. Michelow, Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa.
Tel.: +27 11 4899099; Fax: +27 11 489 9411
E‐mail: <email>pamela.michelow@nhls.ac.za</email></correspondenceTo><linkGroup><link type="toTypesetVersion" href="file:CYT.CYT474.pdf"></link></linkGroup></publicationMeta><contentMeta><unparsedEditorialHistory>Accepted for publication 30 April 2007</unparsedEditorialHistory><countGroup><count type="figureTotal" number="8"></count><count type="tableTotal" number="2"></count></countGroup><titleGroup><title type="main">The utility of fine needle aspiration in HIV positive children</title><title type="shortAuthors"><b>P. Michelow et al.</b></title><title type="short"><b>Utility of fine needle aspiration in HIV positive children</b></title></titleGroup><creators><creator creatorRole="author" xml:id="cr1" affiliationRef="#a1"><personName><givenNames>P.</givenNames><familyName>Michelow</familyName></personName></creator><creator creatorRole="author" xml:id="cr2" affiliationRef="#a2"><personName><givenNames>T.</givenNames><familyName>Meyers</familyName></personName></creator><creator creatorRole="author" xml:id="cr3" affiliationRef="#a1"><personName><givenNames>M.</givenNames><familyName>Dubb</familyName></personName></creator><creator creatorRole="author" xml:id="cr4" affiliationRef="#a3"><personName><givenNames>C.</givenNames><familyName>Wright</familyName></personName></creator></creators><affiliationGroup><affiliation xml:id="a1" countryCode="ZA"><unparsedAffiliation>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa</unparsedAffiliation></affiliation><affiliation xml:id="a2" countryCode="ZA"><unparsedAffiliation>Harriet Shezi Children’s Clinic, Department of Paediatrics, Chris Hani Baragwanath Hospital, and University of the Witwatersrand, Johannesburg, South Africa</unparsedAffiliation></affiliation><affiliation xml:id="a3" countryCode="ZA"><unparsedAffiliation>Department of Anatomical Pathology, Tygerberg hospital, National Health Laboratory Service, University of Stellenbosch, Cape Town, South Africa</unparsedAffiliation></affiliation></affiliationGroup><keywordGroup xml:lang="en"><keyword xml:id="k1">fine needle aspirates</keyword><keyword xml:id="k2">human immunodeficiency virus</keyword><keyword xml:id="k3">paediatric population</keyword><keyword xml:id="k4">reactive lymphadenopathy</keyword><keyword xml:id="k5">mycobacterial infection</keyword><keyword xml:id="k6">cytodiagnosis</keyword><keyword xml:id="k7">cytological technique</keyword><keyword xml:id="k8">laboratory diagnosis</keyword></keywordGroup><abstractGroup><abstract type="main" xml:lang="en"><!--
P. Michelow, T. Meyers, M. Dubb and C. Wright
The utility of fine needle aspiration in HIV positive children
--><p><b>Objective: </b> To determine the spectrum of disease, diagnostic accuracy and adequacy of fine needle aspirates (FNA) in human immunodeficiency virus (HIV) positive children who present with mass lesions.</p><p><b>Methods: </b> Between January 1997 and December 2002, 95 FNAs were performed in 91 children aged 15 years and younger who were known to be infected with the human immunodeficiency virus (HIV).</p><p><b>Results: </b> Head and neck masses including salivary gland swellings were the most common presentation (58.9%) followed by axillary masses (25.3%). Groin masses were aspirated in six children, flank and abdominal masses in four children, buttock masses in three children, a chest wall mass in one child and a sonar guided FNA of a lung mass in one child. Eight FNAs (8.4%) proved inadequate. Reactive lymphadenopathy was diagnosed in 42 cases, mycobacterial infection in 22, four children were diagnosed with abscess, one child had a fungal infection and five were found to have non‐Hodgkin’s lymphoma. There were four cases each of lymphoepithelial lesion and Kaposi sarcoma. There was one case each of nephroblastoma, rhabdomyosarcoma, myeloma, melanotic progonoma and spindle cells, not otherwise specified.</p><p><b>Conclusion: </b> Fine needle aspiration in HIV positive children is a worthwhile procedure and in most instances allows a rapid diagnosis obviating the need for surgery and enabling swift treatment to be undertaken where necessary. Ancillary studies form an important diagnostic component. Universal safety precautions must be strictly adhered to.</p></abstract></abstractGroup></contentMeta></header></component></istex:document></istex:metadataXml><mods version="3.6"><titleInfo lang="en"><title>The utility of fine needle aspiration in HIV positive children</title></titleInfo><titleInfo type="abbreviated" lang="en"><title>Utility of fine needle aspiration in HIV positive children</title></titleInfo><titleInfo type="alternative" contentType="CDATA" lang="en"><title>The utility of fine needle aspiration in HIV positive children</title></titleInfo><name type="personal"><namePart type="given">P.</namePart><namePart type="family">Michelow</namePart><affiliation>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa</affiliation><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">T.</namePart><namePart type="family">Meyers</namePart><affiliation>Harriet Shezi Children’s Clinic, Department of Paediatrics, Chris Hani Baragwanath Hospital, and University of the Witwatersrand, Johannesburg, South Africa</affiliation><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">M.</namePart><namePart type="family">Dubb</namePart><affiliation>Cytology Unit, National Health Laboratory Service and University of the Witwatersrand, Johannesburg, South Africa</affiliation><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">C.</namePart><namePart type="family">Wright</namePart><affiliation>Department of Anatomical Pathology, Tygerberg hospital, National Health Laboratory Service, University of Stellenbosch, Cape Town, South Africa</affiliation><role><roleTerm type="text">author</roleTerm></role></name><typeOfResource>text</typeOfResource><genre type="article" displayLabel="article" authority="ISTEX" authorityURI="https://content-type.data.istex.fr" valueURI="https://content-type.data.istex.fr/ark:/67375/XTP-6N5SZHKN-D">article</genre><originInfo><publisher>Blackwell Publishing Ltd</publisher><place><placeTerm type="text">Oxford, UK</placeTerm></place><dateIssued encoding="w3cdtf">2008-04</dateIssued><edition>Accepted for publication 30 April 2007</edition><copyrightDate encoding="w3cdtf">2008</copyrightDate></originInfo><language><languageTerm type="code" authority="rfc3066">en</languageTerm><languageTerm type="code" authority="iso639-2b">eng</languageTerm></language><physicalDescription><extent unit="figures">8</extent><extent unit="tables">2</extent></physicalDescription><abstract>Objective: To determine the spectrum of disease, diagnostic accuracy and adequacy of fine needle aspirates (FNA) in human immunodeficiency virus (HIV) positive children who present with mass lesions.</abstract><abstract>Methods: Between January 1997 and December 2002, 95 FNAs were performed in 91 children aged 15 years and younger who were known to be infected with the human immunodeficiency virus (HIV).</abstract><abstract>Results: Head and neck masses including salivary gland swellings were the most common presentation (58.9%) followed by axillary masses (25.3%). Groin masses were aspirated in six children, flank and abdominal masses in four children, buttock masses in three children, a chest wall mass in one child and a sonar guided FNA of a lung mass in one child. Eight FNAs (8.4%) proved inadequate. Reactive lymphadenopathy was diagnosed in 42 cases, mycobacterial infection in 22, four children were diagnosed with abscess, one child had a fungal infection and five were found to have non‐Hodgkin’s lymphoma. There were four cases each of lymphoepithelial lesion and Kaposi sarcoma. There was one case each of nephroblastoma, rhabdomyosarcoma, myeloma, melanotic progonoma and spindle cells, not otherwise specified.</abstract><abstract>Conclusion: Fine needle aspiration in HIV positive children is a worthwhile procedure and in most instances allows a rapid diagnosis obviating the need for surgery and enabling swift treatment to be undertaken where necessary. Ancillary studies form an important diagnostic component. Universal safety precautions must be strictly adhered to.</abstract><subject lang="en"><genre>keywords</genre><topic>fine needle aspirates</topic><topic>human immunodeficiency virus</topic><topic>paediatric population</topic><topic>reactive lymphadenopathy</topic><topic>mycobacterial infection</topic><topic>cytodiagnosis</topic><topic>cytological technique</topic><topic>laboratory diagnosis</topic></subject><relatedItem type="host"><titleInfo><title>Cytopathology</title></titleInfo><genre type="journal" authority="ISTEX" authorityURI="https://publication-type.data.istex.fr" valueURI="https://publication-type.data.istex.fr/ark:/67375/JMC-0GLKJH51-B">journal</genre><identifier type="ISSN">0956-5507</identifier><identifier type="eISSN">1365-2303</identifier><identifier type="DOI">10.1111/(ISSN)1365-2303</identifier><identifier type="PublisherID">CYT</identifier><part><date>2008</date><detail type="volume"><caption>vol.</caption><number>19</number></detail><detail type="issue"><caption>no.</caption><number>2</number></detail><extent unit="pages"><start>86</start><end>93</end><total>8</total></extent></part></relatedItem><identifier type="istex">57FD5B2DC4DD2C47C242710C928FB67C60BF420B</identifier><identifier type="ark">ark:/67375/WNG-0N94MRFR-T</identifier><identifier type="DOI">10.1111/j.1365-2303.2007.00474.x</identifier><identifier type="ArticleID">CYT474</identifier><accessCondition type="use and reproduction" contentType="copyright">© 2007 National Health Laboratory Service</accessCondition><recordInfo><recordContentSource authority="ISTEX" authorityURI="https://loaded-corpus.data.istex.fr" valueURI="https://loaded-corpus.data.istex.fr/ark:/67375/XBH-L0C46X92-X">wiley</recordContentSource><recordOrigin>Blackwell Publishing Ltd</recordOrigin></recordInfo></mods><json:item><extension>json</extension><original>false</original><mimetype>application/json</mimetype><uri>https://api.istex.fr/document/57FD5B2DC4DD2C47C242710C928FB67C60BF420B/metadata/json</uri></json:item></metadata><serie></serie></istex></record>Pour manipuler ce document sous Unix (Dilib)
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