Flow Cytometric Detection of CD79a Expression in T-Cell Acute Lymphoblastic Leukemias

Lai, Raymond; Juco, Jonathan; Lee, Siow Fong; Nahirniak, Susan; Etches, Wai S.

doi:10.1309/391r-93yf-db4d-1l35

Cited by 47 publications

(30 citation statements)

References 20 publications

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“…4,5 It is considered to represent a B lineage restricted marker, 6 although weak cCD79a expression has been detected by immunohistochemistry or flow cytometry in 10-40% of a limited number of T-ALLs. [7][8][9][10] Incomplete immunoglobulin (Ig) DJ rearrangements first occur in CD34 þ , CD19À, CD10 þ , cCD79a þ early B cells, whereas VDJ rearrangements commence in CD19 þ , pro-B cells, just prior to appearance of cytoplasmic Igm and pre-BCR expression. [11][12][13] Whether the earliest IgH DJ rearranged, CD79a þ precursors are B lymphoid restricted is not clear.…”

Section: Introductionmentioning

confidence: 99%

IgH DJ rearrangements within T-ALL correlate with cCD79a expression, an immature/TCRγδ phenotype and absence of IL7Rα/CD127 expression

et al. 2004

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cCD79a and IgH VDJ/DJ rearrangements are considered to be relatively specific for B lymphoid precursors. We looked for both in cCD3 þ , CD7 þ , CD19-T-ALLs classified by TCR status into ab or cd/immature (IM) lineages, with individualization of HOX11L2 þ T-ALLs since they represent an intermediate ab/cd category. cCD79a was expressed at low levels in 47% of T-ALL and was most frequent in IMc T-ALLs. IgH rearrangements were common in cd/IM (45%) and HOX11L2 þ (35%) T-ALLs compared to HOX11L2-negative cases (3%; Po0.001). CD127 (IL7Ra) expression was also more common in the cd/IM lineage but its expression was virtually mutually exclusive of IgH rearrangement. Low-level cCD79a expression alone should therefore not be interpreted as evidence of B lineage affiliation in immature leukemias. cd/IM lineage T-ALLs potentially include two distinct categories: predominantly IgH þ , cCD79a þ , CD127-cases which retain cd and B lymphoid potential and IgHÀ, cCD79aÀ, CD127 þ cases with restricted T lineage potential.

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Section: Introductionmentioning

confidence: 99%

IgH DJ rearrangements within T-ALL correlate with cCD79a expression, an immature/TCRγδ phenotype and absence of IL7Rα/CD127 expression

et al. 2004

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“…The majority of B-lineage acute lymphoblastic leukaemias (ALL) are CD79a-positive while reactions are usually negative in acute myeloid leukaemias (AML) (Buccheri et al, 1993). Although there have been two reports describing CD79a expression in T lineage ALL (Pilozzi et al, 1998;Lai et al, 2000), the signi®cance of these ®ndings is still uncertain. One of the two studies (Lai et al, 2000) documented three T-ALL cases whose cells expressed CD79a weakly.…”

mentioning

confidence: 99%

“…Although there have been two reports describing CD79a expression in T lineage ALL (Pilozzi et al, 1998;Lai et al, 2000), the signi®cance of these ®ndings is still uncertain. One of the two studies (Lai et al, 2000) documented three T-ALL cases whose cells expressed CD79a weakly. However, two of these cases were also CD10-positive qualifying as biphenotypic acute leukaemia (B plus T lymphoid) (Matutes et al, 1997;Bene et al, 1998b;Brunning et al, 2001).…”

mentioning

confidence: 99%

Revised guideline on immunophenotyping in acute leukaemias and chronic lymphoproliferative disorders

Bain

Barnett

Linch

et al. 2002

Clinical &Amp; Laboratory Haematology

100

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“…CD79a is a highly lineage-specific marker of B lymphoid cells and plays an important role in the diagnosis of acute leukemia [42]. In this study 33% of B-ALL cases express CD79a.…”

Section: Acute Lymphoblastic Leukemia (All)mentioning

confidence: 62%

Immunophenotypic Profile in Adult Patients with Acute Leukemia Association with Clinical Feature: Fluorescence Cytometry Quantitative Analysis

Elbossaty¹

2017

J Mol Biomark Diagn

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Antigen surface markers represent as the new prognostic tool for detection of acute leukemia. To investigate the prevalence expression of lymphoid and myeloid antigen lineage in acute leukemias. This study included 100 acute leukemias patients. Specimens were selected from consecutive patients who had sufficient material available. Among the 100 patients in which a detailed history, hematological, clinical and immunophenotyping analysis were performed. This study was showed distribution of immunophenotyping characters between studied AML and ALL cases. The most abundant immunophenotyping features in acute myeloid leukemia were cMPO, CD33, CD117, CD13, CD14 and CD64, while the most abundant immunophenotyping features in acute lymphoblastic leukemia were CD19, CD79a, TdT, CD20, CD10 and CD34. cMPO which act as independent prognostic factor for AML, CD10 and TdT can used as independent prognostic factor for differentiate between ALL and AML.

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Flow Cytometric Detection of CD79a Expression in T-Cell Acute Lymphoblastic Leukemias

Cited by 47 publications

References 20 publications

IgH DJ rearrangements within T-ALL correlate with cCD79a expression, an immature/TCRγδ phenotype and absence of IL7Rα/CD127 expression

IgH DJ rearrangements within T-ALL correlate with cCD79a expression, an immature/TCRγδ phenotype and absence of IL7Rα/CD127 expression

Revised guideline on immunophenotyping in acute leukaemias and chronic lymphoproliferative disorders

Immunophenotypic Profile in Adult Patients with Acute Leukemia Association with Clinical Feature: Fluorescence Cytometry Quantitative Analysis

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