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20881

Role of CD11a and CD18 in Diagnosis of Acute Promyelocytic Leukemia

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Last updated: 24 Dec 2024

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Abstract

Background: Acute promyelocytic leukemia (APL) is an aggressive subtype of acute myeloid leukemia (AML) that requires rapid diagnosis and early intervention. Previous studies spotted light on APL being negative for members of β2 integrin family CD11a and CD18. The aim of this work: was to study the value of absence of CD11a and CD18 molecules in screening and its relation to prognosis of APL cases. Patients and methods: This cross sectional study was conducted on seventy adult (>18 years) patients with de novo AML, recruited from National Cancer Institute, Cairo University. They were divided in to 2 groups; group 1 of APL cases (n= 35) and group 2 of AML-Non APL cases (n= 35) as a comparative group. Both groups were investigated by flow cytometry for the expression of CD11a and CD18 molecules on leukemic cells. Results: Comparison between group 1 and group 2 illustrated significant reduction in % of cells expressing CD11a (p= 0.014), CD18 (p=0.008) and % of cells co-expressing CD11a /CD18 (p=0.007) in group 1 compared to group 2. There was significant positive correlation between % of cells expressing CD18 and TLC (r=0.411, p=0.014). There was significant positive correlation between CD11a MFI and hepatomegaly (r=0.390, p=0.021) in AML-Non APL group. Regarding the output data of ROC curve for discriminative percentage of leukemic cells expressing CD11a and CD18 between APL and Non-APL groups, at cut off 78.95% and 23.5% respectively, the specificity for both was 60% and 68.6%, respectively. While sensitivity was 77.1% and 68.6%, respectively, with Area Under Curve (AUC) of 0.671 and 0.686 and p value of 0.014, and 0.008 for leukemic cells expressing CD11a and CD18, respectively. Conclusion: [1] There is significant reduction in % of cells expressing CD11a and CD18 in APL patients, but they were neither sensitive nor specific to be used as single markers in diagnosis of APL patients. [2] Positive correlation seen between the most important prognostic factor, TLC and both CD18 MFI and percentage of cells expressing CD18 could throw light on the potentiality of CD18 as a prognostic factor. [3] Significant positive correlation between CD11a MFI and hepatomegaly in Non-APL cases might suggest a role of CD11a in migration of leukemic cells.

DOI

10.21608/ejhm.2018.20881

Keywords

APL, AML, CD11a, CD18

Authors

First Name

Mona H.

Last Name

Alrayes

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Affiliation

Department of Clinical Pathology, Faculty of Medicine for Girls, Al-Azhar University

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First Name

Reham H.M.

Last Name

Hammad

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Affiliation

Department of Clinical Pathology, Faculty of Medicine for Girls, Al-Azhar University

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Orcid

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First Name

Enas M.

Last Name

Radwan

MiddleName

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Affiliation

Department of Clinical Pathology National Cancer Institute (NCI), Cairo University

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Orcid

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First Name

Samar M.

Last Name

Abd El-Hamid

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-

Affiliation

Department of Clinical Pathology, Faculty of Medicine for Girls, Al-Azhar University

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Volume

73

Article Issue

11

Related Issue

4124

Issue Date

2018-10-01

Receive Date

2018-12-08

Publish Date

2018-10-01

Page Start

7,939

Page End

7,950

Print ISSN

1687-2002

Online ISSN

2090-7125

Link

https://ejhm.journals.ekb.eg/article_20881.html

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https://ejhm.journals.ekb.eg/service?article_code=20881

Order

11

Type

Original Article

Type Code

606

Publication Type

Journal

Publication Title

The Egyptian Journal of Hospital Medicine

Publication Link

https://ejhm.journals.ekb.eg/

MainTitle

Role of CD11a and CD18 in Diagnosis of Acute Promyelocytic Leukemia

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Article

Created At

22 Jan 2023