TY  - BOOK
AU  - Aya Mansour Hassan Ahmed,
AU  - Manal Mohamed Mahmoud Makhlouf 
AU  - Kareeman Gomaa Mohammed 
AU  - Yasmeen Mohammed Mahmoud Selim 
TI  - Association of CD247 single nucleotide gene variant with immune thrombocytopenic purpura among egyptian children
U1  - 612.117 
PY  - 2024///
KW  - Thrombocytopenia
KW  - qrmak
KW  - Immune thrombocytopenic purpura
KW  - CD247 rs858554
KW  - gene variants
KW  - Taqman RT-PCR
N1  - Thesis (M.Sc)-Cairo University, 2024; Bibliography: pages 110-119; Issues also as CD
N2  - Background: Immune Thrombocytopenic Purpura (ITP) is an autoimmune disorder characterized by abnormal immune response leading to a low circulating platelet count due to increased platelets destruction as well as suboptimal platelets production. CD247 is a component of T cell receptor that plays an important role in assembly and transport of the TCR/CD3 complex to the cell surface and in receptor signaling functions. CD247 rs858554 has been reported and is shown to impair immune functions, suggesting the potential involvement in the pathogenesis of autoimmune diseases including ITP.
Aim of the Work: The present work was done to study the prevalence and the possible relation between CD247 rs858554 single nucleotide variant and ITP disease in a cohort of Egyptian children, and to describe the correlation of this variant with the demographic, clinical and laboratory findings, response to treatment and prognosis of the patients, as well as to clarify the ability of using this variant in risk stratification of ITP disease
Participants and Methods: Seventy patients with ITP as well as 70 age and sex matched normal healthy controls were included. CD247 rs858554 G-to-A was determined by allelic discrimination Taqman real-time PCR. 
Results: Our study revealed that CD247 rs858554 G>A variants among ITP patients were found to be GG genotype (41%), AG (46%) and AA (13%), while among the control group were GG (40%), AG (44%) and AA (16%) with no statistically significant difference between the 2 groups (p Ë0.05) and that CD247 rs858554 variants had no role as a risk factor of ITP susceptibility whether acute or chronic ITP. Regarding prognosis of ITP patients who were responsive to steroids were found to be GG (43%), AG (45%) and AA (12%), while among the irresponsive ITP were GG (33%), AG (50%) and AA (17%) with no significant difference between the 2 groups (p Ë0.05) and that CD247 rs858554 variants had no impact on prognosis or treatment outcome. 
Conclusion: CD247 rs858554 had no role in ITP susceptibility, disease severity or prognosis.; ÙØªÙÙØ² ÙØ±Ø¶ ÙÙØµ Ø§ÙØµÙØ§Ø¦Ø­ Ø§ÙØ¯ÙÙÙØ© Ø§ÙÙÙØ§Ø¹Ù Ø¨Ø£Ø¶Ø·Ø±Ø§Ø¨ ÙÙ Ø§ÙÙÙØ§Ø¹Ø© Ø§ÙØ°Ø§ØªÙØ© ÙØªÙØ¬Ø© ÙÙØ¬ÙØ¯ Ø£Ø¬Ø³Ø§Ù ÙØ¶Ø§Ø¯Ø© ÙÙØµÙØ§Ø¦Ø­ Ø§ÙØ¯ÙÙÙØ© ÙÙÙÙØ³ØªØ¶Ø¯ Ø§ÙØ®Ø§Øµ Ø¨Ø®ÙØ§ÙØ§ Ø§ÙØªÙ Ø§ÙÙÙÙÙØ§ÙÙØ© ÙØ§ÙØ°Ù ÙÙÙÙ Ø£Ù ÙØªØ³Ø¨Ø¨ ÙÙ ØªØ¯ÙÙØ± Ø§ÙØ·Ø­Ø§Ù Ø§ÙØ·Ø±ÙÙ ÙÙØµÙØ§Ø¦Ø­ Ø§ÙØ¯ÙÙÙØ© Ø£Ù Ø¥Ø¹Ø§ÙØ© ØªØ®ÙÙÙ Ø§ÙØµÙØ§Ø¦Ø­ Ø§ÙØ¯ÙÙÙØ© ÙÙ Ø§ÙÙØ®Ø§Ø¹ Ø§ÙØ¹Ø¸ÙÙ. ÙØ¹ÙÙ Ø§ÙØ±ØºÙ ÙÙ Ø§ÙØªÙØ¯Ù ÙÙ ÙÙÙ Ø¢ÙÙØ© ØªØ·ÙØ± ÙØ±Ø¶ ÙÙØµ Ø§ÙØµÙØ§Ø¦Ø­ Ø§ÙØ¯ÙÙÙØ© Ø§ÙÙÙØ§Ø¹ÙØ Ø¥ÙØ§ Ø£Ù Ø§ÙØ¢ÙÙØ© Ø§ÙÙÙØ§Ø¹ÙØ© Ø§ÙØ£ÙÙÙØ© ÙÙÙØ±Ø¶ ÙÙ ÙØªÙ ØªØ­Ø¯ÙØ¯ÙØ§ Ø¨Ø¹Ø¯.
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