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J Vet Sci. 2008 Mar;9(1):45-50 |
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Serum immunoglobulin fused interferon-¥á inhibited tumor growth in athymic mice bearing colon 26 adenocarcinoma cells
Jun-Sung Kim1, Kyeong Nam Yu1, Mi Suk Noh1,2, Min-Ah Woo1,2, Sung-Jin Park1, Jin Hong Park1, Jin Hua1, Hyun Sun Cho1, Soon Kyung Hwang1, Eun-Sun Lee1, Youn-Sun Chung1, In-Young Choi3, Se-Chang Kwon3, Myung-Haing Cho1,2,* |
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1Laboratory of Toxicology, College of Veterinary Medicine and 2Interdisciplinary Program in Nano-Science and Technology, Seoul National University, Seoul 151.742, Korea
3Hanmi Pharmaceutical Research Center, Hwaseong 445-813, Korea
* mchotox@snu.ac.kr |
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Interferon (IFN) has therapeutic potential for a wide range
of infectious and proliferative disorders. However, the
half-life of IFN is too short to have a stable therapeutic effect.
To overcome this problem, serum immunoglobulin has been
fused to IFN. In this study, the efficacy of serum immunoglobulin
fused INFs (si-IFN1 and si-IFN2) was evaluated on
athymic mice bearing colon 26 adenocarcinoma cells. Seven
days after the implantation of tumor cells, each group of
mice was injected once a week with si-IFN1 and si-IFN2 at
two different concentrations (10 ¡¿ : 30 ¥ìg/kg and 50 ¡¿ : 150
¥ìg/kg). A slight anti-tumoral effect was observed in all 10 ¡¿
groups compared to the control. In the 50 ¡¿ groups, however,
si-IFN1 and si-IFN2 showed significant anti- tumoral effects
compared to the control. To gain more information on the
mechanisms associated with the decrease of tumor size, a
Western blot assay of apoptosis-related molecules was
performed. The protein expression of cytochrome c, caspase
9, 6, and 3 were increased by si-IFN1 and si-IFN2. These 2
IFNs also increased the expressions of p53, p21, Bax and
Bad. Interestingly, si-IFN1 and si-IFN2 decreased the
expression of VEGF-¥â. Taken together, serum immunoglobulin
fused IFNs increased therapeutic efficacy under
current experimental condition.
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