TY  - BOOK
AU  - Reham Ahmed Mahdy Hassan,
AU  - Hala Aly Helmy Abdel Rahman
AU  - Mona Salah Eldin Hamdy Abd Elhamid
AU  - Hanan Al-Husseini Al-Wakeel
AU  - Amira Diyaa Darwish
TI  - Expression patterns of immune checkpoints in Egyptian acute myeloid leukemia patients
U1  - 616.99419071 
PY  - 2025///
KW  - myeloid leukemia
KW  - Ø³Ø±Ø·Ø§Ù Ø§ÙØ¯Ù Ø§ÙÙÙÙÙØ¯Ù
KW  - Acute myeloid leukemia (AML)
KW  - Programmed death-1 (PD-1)
KW  - programmed death- ligand-1 (PD-L1)
KW  - Cytotoxic T-cell antigen-4 (CTLA-4)
KW  - Lymphocyte activation gene-3 (LAG-3)
N1  - Thesis (Ph.D)-Cairo University, 2025; Bibliography: pages 149-165; Issues also as CD
N2  - Background: Immune checkpoints such as PD-1, PD-L1, CTLA-4, and LAG-3 regulate immune responses and maintain self-tolerance. Tumor cells can exploit these pathways to evade immune surveillance. Their role in acute myeloid leukemia (AML) is gaining attention, with implications for novel therapeutic strategies. 
Objective: To evaluate the expression of PD-1, PD-L1, CTLA-4, and LAG-3 in adult AML patients and assess correlations with treatment response and clinical features. 
Methods: Fifty-nine newly diagnosed adult AML patients and 20 age- and sexmatched healthy controls were included. mRNA expression levels of immune checkpoints were quantified using TaqMan Real-Time PCR. 
Results: PD-1, PD-L1, CTLA-4, and LAG-3 expression levels were significantly higher in AML patients compared to controls (P < 0.001). Increased expression of PD-1, CTLA-4, and LAG-3 was observed in patients with high leukocyte counts. Positive correlations were found among all four checkpoints, suggesting coordinated regulation. While expression levels were higher in patients with intermediate and adverse risk profiles, however the difference was not statistically significant. No significant association was found between checkpoint expression and response to induction chemotherapy. Additionally, none of the markers independently predicted overall or disease-free survival. 
Conclusion: Immune checkpoint genes are upregulated and co-expressed in AML, indicating a potential role in immune evasion. Although not predictive of treatment response or survival in this cohort, these findings support the need for further investigation of immune checkpoints as potential biomarkers and therapeutic targets in AML, particularly in larger studies.; Ø§ÙØ®ÙÙÙØ©: ØªÙØ¸Ù ÙÙØ§Ø· Ø§ÙØªÙØªÙØ´ Ø§ÙÙÙØ§Ø¹ÙØ©Ø ÙØ«Ù PD-1 ÙPD-L1 ÙCTLA-4 ÙLAG-3Ø Ø§ÙØ§Ø³ØªØ¬Ø§Ø¨Ø§Øª Ø§ÙÙÙØ§Ø¹ÙØ© ÙØªØ­Ø§ÙØ¸ Ø¹ÙÙ ØªØ­ÙÙ Ø§ÙØ°Ø§Øª. ØªØ³ØªØ·ÙØ¹ Ø§ÙØ®ÙØ§ÙØ§ Ø§ÙØ³Ø±Ø·Ø§ÙÙØ© Ø§Ø³ØªØºÙØ§Ù ÙØ°Ù Ø§ÙÙØ³Ø§Ø±Ø§Øª ÙÙØªÙØ±Ø¨ ÙÙ Ø§ÙÙØ±Ø§ÙØ¨Ø© Ø§ÙÙÙØ§Ø¹ÙØ©. ÙØªØ²Ø§ÙØ¯ Ø§ÙØ§ÙØªÙØ§Ù Ø¨Ø¯ÙØ±ÙØ§ ÙÙ Ø§Ø¨ÙØ¶Ø§Ø¶ Ø§ÙØ¯Ù Ø§ÙÙØ®Ø§Ø¹Ù Ø§ÙØ­Ø§Ø¯ (AML)Ø ÙÙØ§ ÙÙØ³ÙÙ ÙÙ ØªØ·ÙÙØ± Ø§Ø³ØªØ±Ø§ØªÙØ¬ÙØ§Øª Ø¹ÙØ§Ø¬ÙØ© Ø¬Ø¯ÙØ¯Ø©.

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