Publications

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2022
Ibrahim, N. S., M. M. Makhlouf, G. H. Shahin, M. K. E. Ghamrawy, and N. M. Hussein, "The impact of MCP1-2518A/G and CCR2-V64I genetic polymorphisms in Egyptian sickle cell disease patients", Experimental and Molecular Pathology, vol. 128, pp. 104834, 2022.
Makhlouf, M. M., M. A. Ayoub, and D. F. Mourad, "The risk and prognostic influence of caspase 9 promotor polymorphisms in Egyptian patients with acute myeloid leukemia", Journal of Hematopathology, vol. 15, pp. 131-140, 2022.
2021
Makhlouf, M. M., E. R. Radwan, O. M. Khorshed, L. M. Fathi, and M. M. Elmasry, "CXC Chemokine Receptor Type 5 Gene Polymorphisms in a Cohort of Egyptian Patients with Diffuse Large B-Cell Lymphoma.", Pathobiology : journal of immunopathology, molecular and cellular biology, vol. 88, issue 3, pp. 211-217, 2021. Abstract

BACKGROUND: The chemokine receptor CXCR5 is selectively expressed on B cells; it is involved in lymphocyte homing and the development of normal lymphoid tissue. Its principle ligand is CXCL13 or B lymphocyte chemoattractant. Three polymorphisms in the CXCR5 gene, rs148351692 C/G, rs6421571 C/T, and rs78440425 G/A, have been identified.

OBJECTIVE: To assess the genetic polymorphisms of CXCR5 and evaluate their possible contribution to the susceptibility and response to therapy of diffuse large B-cell lymphoma (DLBCL).

PATIENTS AND METHODS: Fifty DLBCL (not otherwise specified) patients and 50 control subjects were included in this study. CXCR5 genotypes were determined by PCR-RFLP.

RESULTS: Our study revealed that the CXCR5 rs148351692 C/G and rs6421571 C/T gene polymorphisms are associated with an increased risk of developing DLBCL (OR 28.57 [95% CI 8.96-96.56] and 3.45 [1.67-11.83] respectively), while CXCR5 rs78440425 G/A showed no association with the risk of lymphoma. Moreover, the double and triple combined gene polymorphisms are associated with an increased risk of developing DLBCL of approximately 120-fold and 105-fold, respectively. CXCR5 gene polymorphisms had no significant impact on disease outcome or response to therapy.

CONCLUSIONS: CXCR5 gene polymorphisms could be considered a potential risk factor for the development of DLBCL.

Mousa, S. M., M. M. Makhlouf, E. T. Mohammed, and H. M. Zawam, "The Influence of Gene Polymorphisms on the Risk and Clinical Outcome of Non-Hodgkin Lymphoma.", Indian journal of hematology & blood transfusion : an official journal of Indian Society of Hematology and Blood Transfusion, vol. 37, issue 4, pp. 549-554, 2021. Abstract

Polymorphisms in the gene are associated with various diseases and cancers including non-Hodgkin lymphoma (NHL). The aim of the study is to assess the impact of genetic polymorphisms [- 330 T/G (rs2069762) and + 114 T/G (rs2069763)] on the susceptibility and prognosis of NHL. Sixty patients with NHL as well as 60 age and sex matched healthy control subjects are included in this study. genotypes were determined by Polymerase Chain Reaction-Restriction Fragment length Polymorphism assay (PCR-RFLP). Our study revealed that both rs2069762 and rs2069763 gene polymorphisms are associated with increased risk of developing NHL; OR = 3.609 (95% CI = 1.527-8.417) and 4.142 (95% CI = 1.637-10.538) respectively. Moreover, the simultaneous presence of both polymorphisms is associated with about 6 fold increased risk of developing NHL. Also, rs2069762 and rs2069763 gene polymorphisms increase the risk of unfavorable prognosis with OR = 17.300 (95% CI = 3.392-87.725) and 10.424(95% CI = 1.870-58.413) respectively. These findings suggest that (rs2069762) and (rs2069763) gene polymorphisms could be involved in the development of NHL.

2020
Abbas, O. M., K. A. Khalifa, M. M. Makhlouf, N. F. Osman, W. M. Abdel Razek, and A. S. Atta, "Influence of esophageal variceal bleeding on iron status in chronic hepatitis C patients", European Journal of Gastroenterology & Hepatology, vol. 32, issue 5, pp. 616-622, 2020.
2017
Makhlouf, M. M., S. G. Elwakil, and N. S. Ibrahim, "Molecular and serological assessment of parvovirus B-19 infection in Egyptian children with sickle cell disease", Journal of Microbiology, Immunology and Infection, vol. 50, issue 5, pp. 565-569, 2017.
Hamdy, M. S. A., Z. A. El-Saadany, M. M. Makhlouf, A. I. Salama, N. S. Ibrahim, and A. A. Gad, "TAp73 and ΔNp73 relative expression in Egyptian patients with lymphoid neoplasms.", Tumori Journal, vol. 103, issue 3, pp. 268-271, 2017.
2016
Makhlouf, M. M., and R. I. Magdy, "The clinical relevance and prognostic significance of microsomal epoxide hydrolase gene polymorphisms and their susceptibility to acquired aplastic anemia: an Egyptian study.", Biomarkers : biochemical indicators of exposure, response, and susceptibility to chemicals, vol. 21, issue 5, pp. 416-23, 2016 Jul. Abstract

BACKGROUND: Microsomal epoxide hydrolase enzyme (mEPHX) is involved in xenobiotics detoxification. Two variants of mEPHX, Tyr113His and His139Arg, have been described. Both may lead to acquired aplastic anemia (AA).

OBJECTIVES: Assessing mEPHX genetic polymorphisms and detecting their impact on susceptibility and prognosis in Egyptian AA patients.

PARTICIPANTS AND METHODS: mEPHX 113 and 139 genotypes were determined by polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) in 100 patients with AA and 100 control subjects.

RESULTS: Both mEPHX Tyr113His and His139Arg gene polymorphisms were associated with increased risk of developing AA, and have a significant impact of bad prognosis (p value < 0.01).

CONCLUSIONS: These mEPHX gene polymorphisms can be considered as risk factors and predictive molecular markers for prognosis in AA patients.

Hamdy, M. S. E. - D., A. S. Nasr, M. M. Makhlouf, Z. A. E. - Saadany, M. Samir, and D. S. Morgan, "Impact of Prothrombotic Risk Factors in a Cohort of Egyptian Hemophilia A Patients.", Molecular diagnosis & therapy, vol. 20, issue 2, pp. 151-9, 2016 Apr. Abstract

INTRODUCTION: Hemophilias are a group of related bleeding disorders that show an X-linked pattern of inheritance. The clinical phenotype of severe hemophilia may vary markedly among patients as a result of many factors, including genetic prothrombotic risk factors.

OBJECTIVES: Our objective was to study the incidence of the most common prothrombotic risk factors for additive effects among Egyptian patients with hemophilia A and their impact on clinical phenotype; annual bleeding frequency and severity of hemophilic arthropathy, as well as the effect of a single variation in these patients.

METHODS: This study was carried out in 100 patients with hemophilia A. Genotyping for factor V Leiden (FVL) G1691A, prothrombin G20210A, MTHFR C677T, and A1298C mutations was conducted using a real time-polymerase chain reaction (RT-PCR) assay.

RESULTS: Our study revealed mutations in hemophilia patients as follows: prothrombin G20210A (3 %), FVL (14 %), MTHFR C677T (42 %), and A1298C (59 %). Despite a lack of statistical significance when each gene was analysed separately, heterozygosity of prothrombin G20210A or FVL was always associated with either a mild or moderate, but never a severe, clinical presentation. The lowest bleeding frequency (less than once per month) was identified among patients with two heterozygous variants irrespective of the involved genes. In addition, the incidence of hemarthrosis was significantly higher among patients with a wild genotype of the prothrombin gene and FVL, and the average number of affected joints was significantly higher among patients with wild-type prothrombin and FVL genes than among heterozygous patients.

CONCLUSION: These prothrombotic mutations have a cumulative effect in amelioration of the severity of bleeding in hemophiliacs. The most prominent effect is that of prothrombin G20210A and FVL, while MTHFR C677A and A1298C gene mutations are less conclusive.

Makhlouf, M. M., "Survivin and cyclin E2 genes expression in a cohort of Egyptian acute leukemia patients: Clinical importance and future prospects.", Cancer biomarkers : section A of Disease markers, vol. 16, issue 1, pp. 181-9, 2016. Abstract

BACKGROUND: Abnormalities in the control of apoptosis play an important role in leukemogenesis. Survivin is a member of inhibitor of apoptosis proteins family, it prevents apoptosis by blocking caspase activity and play a role in cell proliferation. While, cyclin E2 is one of the cyclins proteins family that controls progression of cell cycle by activation of cyclin dependant-kinase.

OBJECTIVE: Was to assess survivin and cyclin E2 genes expression in acute leukemia (AL) patients, and to define their role in the susceptibility of AL, and their correlation with the clinical presentation, laboratory findings, as well as treatment outcome.

PATIENTS AND METHODS: This study included 60 de novo AL patients and 40 control subjects to study the expression of survivin and cyclin E2 genes using RT-PCR.

RESULTS: Survivin and cyclin E2 genes expression was significantly higher in leukemic patients compared with control subjects (P< 0.001), both genes separately were associated with increased risk of leukemia development and treatment failure (P< 0.01). Moreover, when combining the 2 genes expression, a significant elevation of the risk of leukemia and treatment failure was found (P < 0.01).

CONCLUSIONS: Survivin and cyclin E2 genes expression may have clinical relevance and can be considered as molecular risk factors for AL. Also they may be useful as predictive markers for treatment outcome in leukemic patients.

2015
Fathy, M. M., M. A. E. Taleb, M. E. S. Hawary, M. I. Nabih, W. M. Aref, and M. M. Makhlouf, "Assessment of interleukin 28B genotype as a predictor of response to combined therapy with pegylated interferon plus ribavirin in HCV infected Egyptian patients", Cytokine, vol. 74, issue 2, pp. 268-272, 2015.
Ibrahim, A. M., N. M. Elgharabawi, M. M. Makhlouf, and O. Y. Ibrahim, "Chondrogenic Differentiation of Human Umbilical Cord Blood-Derived Mesenchymal Stem Cells In Vitro", Microscopy Research and Technique, vol. 78, issue 8, pp. 667-675, 2015.
Kamel, A. K., H. A. M. El-Ghany, M. K. Mekkawy, M. M. Makhlouf, I. M. Mazen, N. El-Dessouky, W. Mahmoud, and S. A. A. El-Kader, "Sex Chromosome Mosaicism in the Gonads of DSD Patients: A Karyotype/ Phenotype Correlation", Sexual Development, vol. 9, issue 5, pp. 279-288, 2015.
Elsaid, A., and M. M. Makhlouf, "Surgical Management of Spontaneous Pyogenic Spondylodiscitis: Clinical and Radiological Outcome", Egyptian Journal of Neurosurgery , vol. 30, issue 3, pp. 221-226, 2015.
2014
Makhlouf, M. M., and S. M. Abdel Hamid, "Expression of IL4 (VNTR intron 3) and IL10 (-627) genes polymorphisms in childhood immune thrombocytopenic purpura.", Laboratory Medicine, vol. 45, issue 3, pp. 211-219, 2014.
2012
Salah Eldin, M., H. N. Raslan, S. M. Abdel Hamid, and M. M. Makhlouf, "Detection of XRCC1 Gene Polymorphisms in Egyptian Patients with Acute Myeloid Leukemia", Comparative Clinical Pathology, 2012.
Kamal, M., Z. Elsaadany, N. Foaad, A. Abel Alaa, M. M. Makhlouf, M. Shaban, and D. Abdel Rahman, "Genetic Polymorphism of Microsomal Epoxide Hydrolase Enzyme Gene in Preeclamptic Females", The American Journal of the Medical Sciences, vol. 343, issue 4, pp. 291-4, 2012.
Ghanem, L. Y., M. M. Nosseir, A. A. Lotfi, A. S. Mohamed, R. A. Ibrahim, M. H. Hassanein, E. Mansour, M. M. Makhlouf, Y. M. Fouad, and H. R. El-Khayat, "Hematopoietic stem cell mobilization into the peripheral circulation in patients with chronic liver diseases", Journal of Digestive Diseases, vol. 13, issue 11, pp. 571-578, 2012.
2011
Farawella, H., H. Zawam, M. M. Makhlouf, N. Bahaa Eldin, and Z. Elsaadany, "Chromosome 20q Aberrations in Philadelphia Positive-Chronic Myeloid Leukemia", Egyptian Journal of Haematology , vol. 36, issue 3, 2011.
Gabr, H., A. Yousry, H. Abou Elghar, Z. Elsaadany, and M. M. Makhlouf, "Derivation of Endothelial Cells from Human Cord Blood CD133+ Cells. ", Egyptian Society of Laboratory Medicine Journal, 2011.
Makhlouf, M. M., "Melanoma Antigen Encoding Gene-A3 Expression, Its Clinical Significance, and Its Risk of Developing Acute Myeloid Leukemia", Journal of Investigative Medicine, vol. 59, issue 7, pp. 1131-6, 2011.
Salah Eldin, M., A. Elhaddad, N. B. Fouad, M. M. Makhlouf, and S. M. Abdel Hamid, "RAD51 and XRCC3 Genes Polymorphisms and the Risk of Developing Acute Myeloid Leukemia.", Journal of Investigative Medicine, vol. 59, issue 7, pp. 1124-30, 2011.
2010
Abdel Rahman, A., S. M. Abdel Hamid, M. M. Makhlouf, N. Eldesouky, M. Elfaky, and S. Yousry, "Detection of CXCL12 Gene Polymorphism and CXCR4 Expression in Egyptian Acute Myeloid Leukemia Patients", Journal of American Science, vol. 6, issue 9, 2010.
2009
Farawella, H., H. Zawam, M. M. Makhlouf, and E. Z.A., "Genomic Aberrations in Egyptian Chronic Lymphocytic Leukemia Patients", Egyptian Society of Haematology & Research Journal, vol. 5, issue 1, 2009.
2008
Nash, S. A., S. M. Abdel Hamid, M. M. Makhlouf, and G. Shaheen, "Expression of JAK2 V617F Mutation in Chronic Myeloproliferative Disorders", Egyptian Society of Laboratory Medicine Journal, vol. 20, issue 3, 2008.