فایل ورد (word) مقاله Anti-tumor Effects of pEgr-1-endostatin-TNF-? Recombinant Plasmid Expression Induced by Ionizing Radiation

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 فایل ورد (word) مقاله Anti-tumor Effects of pEgr-1-endostatin-TNF-? Recombinant Plasmid Expression Induced by Ionizing Radiation دارای 8 صفحه می باشد و دارای تنظیمات در microsoft word می باشد و آماده پرینت یا چاپ است

فایل ورد فایل ورد (word) مقاله Anti-tumor Effects of pEgr-1-endostatin-TNF-? Recombinant Plasmid Expression Induced by Ionizing Radiation  کاملا فرمت بندی و تنظیم شده در استاندارد دانشگاه  و مراکز دولتی می باشد.

توجه : در صورت  مشاهده  بهم ريختگي احتمالي در متون زير ،دليل ان کپي کردن اين مطالب از داخل فایل ورد مي باشد و در فايل اصلي فایل ورد (word) مقاله Anti-tumor Effects of pEgr-1-endostatin-TNF-? Recombinant Plasmid Expression Induced by Ionizing Radiation،به هيچ وجه بهم ريختگي وجود ندارد

بخشی از متن فایل ورد (word) مقاله Anti-tumor Effects of pEgr-1-endostatin-TNF-? Recombinant Plasmid Expression Induced by Ionizing Radiation :


سال انتشار : 2011

تعداد صفحات :8

Purpose: The aim of the present study was to investigate the anti-tumor effect of a pEgr-1-endostatin-TNF- recombinant plasmid induced by ionizing radiation. Method: Three hundred and twenty mice bearing Lewis lung carcinomas were divided into four experimental groups: blank control, irradiation treatment, plasmid treatment and plasmid combined irradiation treatment. Twenty-four hours after the recombinant plasmid was injected locally into the tumors of the mice, they were irradiated with 10 Gy -rays. The concentration of TNF- and endostatin in the serum of mice was measured by ELISA and tumor growth in each group was compared. The tumor microvessel density was examined by H&E staining and immunohistochemistry analysis of CD31 positive cells. Results: Radiation could induce the expression of pEgr-1-endostatin-TNF. The levels of endostatin and TNF- could express steadily for about 4 weeks, with concentrations of 52.6±4.19 and 12.0±0.87 ng/ml respectively, in the second week in combined therapy group and maintained at relative higher level in the fourth week than other groups (F=29.7, P<0.05). Compared with the control group, the tumor micro vessel density was significantly depressed (P<0.05) and tumor growth was significantly inhibited (5907.2±78.6 mm3 vs. 763.5±12.3 mm3, P <0.05). Conclusions: The expression of pEgr-1-endostatin-TNF- could be induced in mice in vivo and exhibited more significant anti-tumor and anti-angiogenesis effects than irradiation alone.

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