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〓猪哥哥〓
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SCI与国内核心期刊差异挺大。
一个是编排格式
一个是写作方式
一个是内容丰度程度。

介绍的是一个脂质体的文章。

《小鼠腹腔注射给药脂质体大小对腹膜的滞留和器官分布的影响》

Effect of liposome size on peritoneal retention and organ distribution after intraperitoneal injection in mice

Abstract

Peritoneal carcinomatosis is a serious concern when treating digestive or ovarian tumors. Treatment with systemic chemotherapy suffers from poor penetration of cytotoxic agents into the peritoneal cavity and is not quite effective. Local delivery of drugs, especially as controlled-release delivery systems like liposomes, could provide sustained and higher drug levels and reduce systemic toxicity.

In order to investigate the effect of liposome size on peritoneal retention, liposomes composed of distearoylphosphatidylcholine and cholesterol (DSPC/CHOL, molar ratio 2:1) were prepared at four sizes of 100, 400, 1000 and 3000 nm. Subsequently, these liposomes were labeled with 99mTc complex of hexamethylpropyleneamineoxime (99mTc-HMPAO) and injected into mouse peritoneum. Then, mice were sacrificed at eight different time points and the percentage of injected radiolabel in the peritoneal cavity and the organ distribution in terms of percentage injected dose/gram tissue (%ID/g) were obtained.

Results showed that the free label (99mTc-HMPAO) was cleared very rapidly from the cavity so that after 5 min and 7 h only 6.89 ± 2.51% and 0.91 ± 0.51% of the injected dose was recovered, respectively. However, for the liposomal formulations, this recovery value ranged from 8.47 ± 1.62% to 29.99 ± 12.06% at 7 h. Peritoneal retention of the vesicles was increased with their size, and the highest retention rate was obtained with 1000 nm liposomes with an AUC value 15.51 times that of 99mTc-HMPAO. In blood, as expected, 100 nm liposomes showed much higher levels because of their greater stability. Their greater blood concentration also caused increased levels in the heart and kidneys, although their organ to blood AUC ratio was the lowest.

Overall, among the different sized neutral liposomes investigated, the 1000 nm vesicles seemed to be the most optimal, achieving a greater peritoneal level and retention.

Keywords: Liposomes; Size; 99mTc-HMPAO; Peritoneal retention; Peritoneal carcinomatosis

Abbreviations: DSPC, distearoylphosphatidylcholine; DMPC, dimiristoylphosphatidylcholine; DMPG, dimiristoylphosphatidylglycerol; CHOL, cholesterol; DOX, doxorubicin; L-NDDP, cis-bis-neodecanoato (trans-R, R-1, 2-diaminocyclohexane)-platinum II entrapped in multilamellar vesicles; HMPAO, hexamethylpropyleneamineoxime; MLV, multilamellar vesicles
该帖子作者被版主 冷冷的冰雨1积分, 2经验,加分理由:谢谢分享
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〓猪哥哥〓
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冷冷的冰雨
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〓猪哥哥〓
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原文由 xy4585618(xy4585618) 发表:
英文看着很费劲啊

如果要知道老外在做些什么,必须要看啊。

多看就会好些
fzhang666
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qqqid
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把西医的研究文章发在“中药分析”版,楼主是来砸场子的???
〓猪哥哥〓
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原文由 qqqid(qqqid) 发表:
把西医的研究文章发在“中药分析”版,楼主是来砸场子的???


就是让大家认识下sci文章。

你还真是喜欢砸场子!
〓猪哥哥〓
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再说脂质体又不是西药才可以做。这个给出的是一个分析方法,对中西药根本没多少涉及。
qqqid
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原文由 〓猪哥哥〓(03yx2) 发表:
再说脂质体又不是西药才可以做。这个给出的是一个分析方法,对中西药根本没多少涉及。

做动物实验、统计学分析,这些都是西药的研究方法,我怕中药也采用洋人的方法,被西药给同化了,我们的传统都保不住了。
lingshike
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青林
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