Effect of some newly synthesized steroid derivatives on apoptosis of breast cancer cells / Ghada Hamdi Elsayed Mohamed ; Supervised Rafat Milad Mohareb , Mervat Sayed Mohamed , Gamal Abdelmegeed Abdelghany

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Ghada Hamdi Elsayed Mohamed

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TextLanguage: English Publication details: Cairo : Ghada Hamdi Elsayed Mohamed , 2017Description: 97 P. : charts , facsimiles ; 25cmOther title:

تأثير بعض المشتقات الستيرويدية الجديدة المشييدة على موت الخلايا المبرمج فى سرطان الثدى [Added title page title]

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Dissertation note: Thesis (Ph.D.) - Cairo University - Faculty of Science - Department of Biochemistry Summary: Anticancer agents consisting of hybrid molecules are used to improve effectiveness and diminish drug resistance. The current study aimed to introduce newly synthesized hetero-steroids of promising anticancer effects. Besides, the pro-apoptotic effects of new compounds were investigated extensively. Several pyrimidino-, triazolopyrimidino-, pyridazino-, and curcumin- steroid derivatives were synthesized, elucidated and confirmed using the spectral and analytical data. The synthesized hetero-steroids, compounds 9, 10, 11, 12, 13, 14, 15, 18, 20, 21, 22 and 24, were tested for their cytotoxic effects versus human breast cancer cells (MCF-7) using neutral red supravital dye uptake assay. Compound 24 (IC50 = 18 æM) showed more inhibitory influence on MCF-7 growth. Using QRT-PCR (Quantitative real time-polymerase chain reaction), CCND1, Survivin, BCL-2, CDC2, P21 and P53, genes expression levels were investigated. The study results disclose that compounds 4, 7, 18, 24 knocked down the expression levels of CCND1, Survivin, BCL-2 and CDC2. However, P21 and P53 were up- regulated by compounds 21, 22. This study introduced promising pro-apoptotic anticancer agents acting through the modulation of key regulators of apoptosis and cell cycle genes. The current study revealed the most promising compounds 7, 18, 21 down-regulated miR-34a, miR-98 and miR-214 expression levels and decreased upon drug resistance response.

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Item type	Current library	Home library	Call number	Copy number	Status	Barcode
Thesis	قاعة الرسائل الجامعية - الدور الاول	المكتبة المركزبة الجديدة - جامعة القاهرة	Cai01.12.02.Ph.D.2017.Gh.E (Browse shelf(Opens below))		Not for loan	01010110072958000
CD - Rom	مخـــزن الرســائل الجـــامعية - البدروم	المكتبة المركزبة الجديدة - جامعة القاهرة	Cai01.12.02.Ph.D.2017.Gh.E (Browse shelf(Opens below))	72958.CD	Not for loan	01020110072958000

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Previous	Cai01.12.02.Ph.D.2017.Em.E The expression of (FLT3, MPL & EPhA4) genes and their relation to prognostic significance in acute myeloid leukemia /	Cai01.12.02.Ph.D.2017.Em.E The expression of (FLT3, MPL & EPhA4) genes and their relation to prognostic significance in acute myeloid leukemia /	Cai01.12.02.Ph.D.2017.Gh.E Effect of some newly synthesized steroid derivatives on apoptosis of breast cancer cells /	Cai01.12.02.Ph.D.2017.Gh.E Effect of some newly synthesized steroid derivatives on apoptosis of breast cancer cells /	Cai01.12.02.Ph.D.2017.Hu.B Biochemical studies on the effect of stem cells treatment in infertile male albino rats /	Cai01.12.02.Ph.D.2017.Hu.B Biochemical studies on the effect of stem cells treatment in infertile male albino rats /	Cai01.12.02.Ph.D.2017.Mo.B Biochemical studies for evaluating the impact of hepatitis C virus co-infection with schistosomiasis on liver fibrosis progression using biotechnology /	Next

Thesis (Ph.D.) - Cairo University - Faculty of Science - Department of Biochemistry

Anticancer agents consisting of hybrid molecules are used to improve effectiveness and diminish drug resistance. The current study aimed to introduce newly synthesized hetero-steroids of promising anticancer effects. Besides, the pro-apoptotic effects of new compounds were investigated extensively. Several pyrimidino-, triazolopyrimidino-, pyridazino-, and curcumin- steroid derivatives were synthesized, elucidated and confirmed using the spectral and analytical data. The synthesized hetero-steroids, compounds 9, 10, 11, 12, 13, 14, 15, 18, 20, 21, 22 and 24, were tested for their cytotoxic effects versus human breast cancer cells (MCF-7) using neutral red supravital dye uptake assay. Compound 24 (IC50 = 18 æM) showed more inhibitory influence on MCF-7 growth. Using QRT-PCR (Quantitative real time-polymerase chain reaction), CCND1, Survivin, BCL-2, CDC2, P21 and P53, genes expression levels were investigated. The study results disclose that compounds 4, 7, 18, 24 knocked down the expression levels of CCND1, Survivin, BCL-2 and CDC2. However, P21 and P53 were up- regulated by compounds 21, 22. This study introduced promising pro-apoptotic anticancer agents acting through the modulation of key regulators of apoptosis and cell cycle genes. The current study revealed the most promising compounds 7, 18, 21 down-regulated miR-34a, miR-98 and miR-214 expression levels and decreased upon drug resistance response.

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