核技术
覈技術
핵기술
NUCLEAR TECHNIQUES
2010年
1期
59-64
,共6页
何佳恒%罗军益%蹇源%王关全%刘国平
何佳恆%囉軍益%蹇源%王關全%劉國平
하가항%라군익%건원%왕관전%류국평
二肽%~(131)I%生物活性
二肽%~(131)I%生物活性
이태%~(131)I%생물활성
Di-peptide%~(131)I%Biodistribution
为了探索前期自行合成的一种碘(~(131)I)代二肽胺作为放射性药物的可能性,本文对其体外稳定性、亲脂性、急性毒性进行了考察.首先采用封管法对二肽胺进行了碘的标记,获得了标记率为85%左右的配合物;通过将配合物放置不同时间测量络合率的变化得到配合物的稳定性结果;采用摇瓶法来考察配合物的亲脂性;对配合物对实验动物的肝脏功能、外周血象的影响作了考察.结果说明,配合物是亲脂性的,毒性较低,3 d后的脱碘率为13%左右.成功建立了VX2肝癌单发肿瘤兔模型,得到了配合物在正常小鼠和肿瘤大白兔体内的分布结果,配合物在动物模型以及在正常小鼠的体内分布趋势比较一致,配合物比较倾向于浓集于脂肪组织,在肿瘤组织中的滞留量相对较高,表现出作为肿瘤治疗药物的潜在可能性,但清除较快,可以作进一步的研究,提高标记物的体内稳定性,以延长配合物在靶向组织中的浓集时间.
為瞭探索前期自行閤成的一種碘(~(131)I)代二肽胺作為放射性藥物的可能性,本文對其體外穩定性、親脂性、急性毒性進行瞭攷察.首先採用封管法對二肽胺進行瞭碘的標記,穫得瞭標記率為85%左右的配閤物;通過將配閤物放置不同時間測量絡閤率的變化得到配閤物的穩定性結果;採用搖瓶法來攷察配閤物的親脂性;對配閤物對實驗動物的肝髒功能、外週血象的影響作瞭攷察.結果說明,配閤物是親脂性的,毒性較低,3 d後的脫碘率為13%左右.成功建立瞭VX2肝癌單髮腫瘤兔模型,得到瞭配閤物在正常小鼠和腫瘤大白兔體內的分佈結果,配閤物在動物模型以及在正常小鼠的體內分佈趨勢比較一緻,配閤物比較傾嚮于濃集于脂肪組織,在腫瘤組織中的滯留量相對較高,錶現齣作為腫瘤治療藥物的潛在可能性,但清除較快,可以作進一步的研究,提高標記物的體內穩定性,以延長配閤物在靶嚮組織中的濃集時間.
위료탐색전기자행합성적일충전(~(131)I)대이태알작위방사성약물적가능성,본문대기체외은정성、친지성、급성독성진행료고찰.수선채용봉관법대이태알진행료전적표기,획득료표기솔위85%좌우적배합물;통과장배합물방치불동시간측량락합솔적변화득도배합물적은정성결과;채용요병법래고찰배합물적친지성;대배합물대실험동물적간장공능、외주혈상적영향작료고찰.결과설명,배합물시친지성적,독성교저,3 d후적탈전솔위13%좌우.성공건립료VX2간암단발종류토모형,득도료배합물재정상소서화종류대백토체내적분포결과,배합물재동물모형이급재정상소서적체내분포추세비교일치,배합물비교경향우농집우지방조직,재종류조직중적체류량상대교고,표현출작위종류치료약물적잠재가능성,단청제교쾌,가이작진일보적연구,제고표기물적체내은정성,이연장배합물재파향조직중적농집시간.
Stability in vitro, lipophility and acute toxicity of p-Boc-Trp-Trp-NH(CH_2)_6NH-PO (ONH_4)-O-Ph~(131)I are studied in this work. The complex, with labeling yield of around 85%, was obtained using sealed-tube method. Stability of the complex was obtained by measuring labeling yield at different time. Its lipophility was studied through swaging-flask method, and its impacts to liver function and peripheral blood of the experimental animals were also studied. The results indicate the complex is lipophilic and less toxic, and the iodine removal rate was about 13% three days later. The rabbit model with VX2 liver tumor was established successfully. The organ and tissue uptake and retention of p-Boc-Trp-Trp-NH(CH_2)_6NH- PO(ONH_4)-O-ph~(131)I were studied in a model subject. Blood, liver, lungs, kidneys, spleen and tumour tissue samples were assayed in a well counter for radioactivity and the results were compared with the biodistribution studies in five normal mice. The complex trends to concentrate into adipose tissues in tumour-bearing and normal animals, and the uptake rate in tumor tissue is relatively high, hence its potential possibility as radiopharmacenticals. But it cleared quickly. Further researches are underway to improve the stability of complexes to prolong concentration time in target tissue.
