Abdelraouf Eldeib scite author profile

Abdelraouf Eldeib

5Publications

12Citation Statements Received

20Citation Statements Given

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Affiliations

Suez Canal University

Publications

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Mechanisms of MCL-1 Protein Stability Induced by MCL-1 Antagonists in B-Cell Malignancies

Tantawy

Sarkar

Hübner

et al. 2022

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Purpose: Several MCL-1 inhibitors (MCL-1i), including AMG-176 and AZD5991, have shown promise in preclinical studies and are being tested for the treatment of hematological malignancies. A unique feature of these agents is induction and stability of Mcl-1 protein; however, the precise mechanism is unknown. We aim to study mechanism of MCL-1i-induced Mcl-1 protein stability. Experimental Design: Using several B-cell leukemia and lymphoma cell lines and primary CLL lymphocytes, we evaluated molecular events associated with Mcl-1 protein stability including protein half-life, reverse-phase protein array, protein-protein interaction, phosphorylation, ubiquitination, deubiquitination, followed by molecular simulation and modeling. Results: Using both in vivo and in vitro analysis, we demonstrate that MCL-1i-induced Mcl-1 protein stability is predominantly associated with defective Mcl-1 ubiquitination and concurrent apoptosis induction in both cell lines and primary CLL subjects. These MCL1i also induced ERK-mediated Mcl-1Thr163 phosphorylation which partially contributed to Mcl-1 stability. Disruption of Mcl-1:Noxa interaction followed by Noxa degradation, enhanced Mcl-1 de-ubiquitination by USP9x, and Mule destabilization are the major effects of these inhibitors. However, unlike other BH3 proteins, Mule:Mcl-1 interaction was unaffected by MCL-1i. WP1130, a global deubiquitinase (DUB) inhibitor, abrogated Mcl-1 induction reaffirming a critical role of DUBs in the observed Mcl-1 protein stability. Further, in vitro ubiquitination studies of Mcl-1 showed distinct difference amongst these inhibitors. Conclusions: We conclude that MCL-1i blocked Mcl-1 ubiquitination via enhanced deubiquitination and dissociation of Mcl-1 from Noxa, Bak and Bax, and Mule de-stabilization. These are critical events associated with increased Mcl-1 protein stability with AMG-176 and AZD5991.

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Assessment of Thyroid Function in Pregnant Females Attending Suez Canal University Hospital

El-Roose

Al-Imam

Eldeib

et al. 2020

Evidence Based Women's Health Journal

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Background: Pregnancy is a physiological state in which significant changes in thyroid function occur. Several factors contribute to these changes. These factors could contribute to thyroid dysfunction during pregnancy especially when a deficiency of iodine intake exists and when thyroid reserve is not sufficient. Aim: To study thyroid functions in pregnant women avoiding maternal and fetal complications associated with thyroid dysfunctions. Materials and Methods: A cross-sectional study was carried out on 100 pregnant women attending Obstetrics Outpatient Clinic in Suez-Canal University Hospitals were invited to enroll in the study. At the end of study, the blood samples were assessed for free T3, free T4 and TSH. Results: This study revealed that most of the pregnant women had normal thyroid functions (51%), while subclinical hypothyroidism (39%) was the most prevalent disorder followed by clinical hypothyroidism (6%) and isolated hypothyroxinemia (4%). Conclusion:The most prevalent pattern of thyroid dysfunction in pregnant women was subclinical hypothyroidism.

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Supplementary Tables S1-S3 from Mechanisms of MCL-1 Protein Stability Induced by MCL-1 Antagonists in B-Cell Malignancies

Tantawy¹,

Sarkar²,

Hübner³

et al. 2023

Preprint

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Supplementary Figures S1-S4 from Mechanisms of MCL-1 Protein Stability Induced by MCL-1 Antagonists in B-Cell Malignancies

Tantawy¹,

Sarkar²,

Hübner³

et al. 2023

Preprint

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Supplementary Methods S1 from Mechanisms of MCL-1 Protein Stability Induced by MCL-1 Antagonists in B-Cell Malignancies

Tantawy¹,

Sarkar²,

Hübner³

et al. 2023

Preprint

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