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作 者:谢建萍[1] 周建亮[1] 刘菲[1] 潘一峰[2] 全俊[1] 谭德明[1]
机构地区:[1]中南大学湘雅医院,湖南长沙410008 [2]卫生部纳米生物技术重点实验室,湖南长沙410008
出 处:《中国医学工程》2007年第4期312-315,共4页China Medical Engineering
基 金:湖南省自然科学基金(No:03JJY3060)
摘 要:目的观察雌二醇纳米粒(E2-PBCA-NP)在正常肝脏中的靶向性,并比较腹腔给药和静脉给药两种给药途径对E2-PBCA-NP肝脏靶向性的影响。方法采用放射示踪技术,用125-I标记雌二醇,界面聚合法制备125-I-E2-PBCA-NP,经腹腔及静脉给药,分别于注药后15、30min、l、2、4、8、l2、24h处死大鼠,取其血、肺、肝、脾、肾、子宫和卵巢作γ计数,并与普通雌二醇组比较。结果125-I-E2-PBCA-NP和125-I-E2肝摄取分别在注射后15min后最高,与125-I-E2比较125-I-E2-PBCA-NP提高了肝脏、脾脏的放射性强度,降低了子宫及卵巢的放射性强度。腹腔给药及尾静脉给药不影响125-I-E2-PBCA-NP的肝脏靶向性(P>0.05)。结论E2-PB-CA-NP具有明显的肝脏靶向性。[Objective] To observe the hepatic targeting of estradiol polybutylcyanoacrylate nanoparticles (E2-PBCA-NP) and compare the effect of hepatic tagerting after intraperitoneal(IP) and intravenous(Ⅳ) administration. [Methods] Using radioactive tracer technique, estradiol labelled with ^125-Ⅰ,^125-Ⅰ-E2-PBCA-NP was prepared by inteffacial polymerization and was injected into mice through IP and Ⅳ administration. At 15, 30 min, 1, 2, 4, 8, 12, 24 h after administration, the mice were sacrificed. The blood,lung, liver, spleen, kidney, ovary and womb were analyzed for γ counts and then compared with common estradiol groups. [Results] ^125-Ⅰ-E2-PBCA-NP and ^125-Ⅰ-E2 uptaken by liver reached the peak at 15 min after administration drugs. Compared with ^125-Ⅰ-E2, ^125-Ⅰ-E2-PBCA-NP enhanced the radioactivity of liver and spleen and reduced the radioactivity of ovary and womb. There was no significant difference on liver targeting after IV or IP administration of ^125-Ⅰ-E,-PBCA-NP (P 〉0.05). [Conclusion] E2- PBCA-NP has remarkable hepatic targeting.
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