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Simultaneous Dual Selective Targeted Delivery of Two Covalent Gemcitabine Immunochemotherapeutics and Complementary Anti-Neoplastic Potency of [Se]-Methylselenocysteine
Simultaneous Dual Selective Targeted Delivery of Two Covalent Gemcitabine Immunochemotherapeutics and Complementary Anti-Neoplastic Potency of [Se]-Methylselenocysteine
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摘要:
The anti-metabolite chemotherapeutic, gemcitabine is relatively effective for a spectrum of neoplastic conditions that include various forms of leukemia and adenocarcinoma/carcinoma. Rapid systemic deamination of gemcitabine accounts for a brief plasma half-life but its sustained administration is often curtailed by sequelae and chemotherapeutic-resistance. A molecular strategy that diminishes these limitations is the molecular design and synthetic production of covalent gemcitabine immunoche-motherapeutics that possess properties of selective “targeted” delivery. The simultaneous dual selective “targeted” delivery of gemcitabine at two separate sites on the external surface membrane of a single cancer cell types represents a therapeutic approach that can increase cytosol chemotherapeutic deposition;prolong chemotherapeutic plasma half-life (reduces administration frequency);minimize innocent exposure of normal tissues and healthy organ systems;and ultimately enhance more rapid and thorough resolution of neoplastic cell populations. Materials and Methods: A light-reactive gemcitabine intermediate synthesized utilizing succinimidyl 4,4-azipentanoate was covalently bound to anti-EGFR or anti-HER2/neu IgG by exposure to UV light (354-nm) resulting in the synthesis of covalent immunoche-motherapeutics, gemcitabine-(C4-amide)-[anti-EGFR] and gemcitabine-(C4-amide)-[anti-HER2/neu]. Cytotoxic anti-neoplastic potency of gemcitabine-(C4-amide)-[anti-EGFR] and gemcitabine-(C4-amide)-[anti-HER2/neu] between?gemcitabine-equivalent concentrations of 10-12 M and 10-6 M was determined utilizing chemotherapeutic-resistant mammary adenocarcinoma (SKRr-3). The organoselenium compound, [Se]-methylselenocysteine was evaluated to determine if it complemented the anti-neoplastic potency of the covalent gemcitabine immunoche-motherapeutics. Results: Gemcitabine-(C4-amide)-[anti-EGFR], gemcitabine-(C4-amide)-[anti-HER2/neu] and the dual simultaneous combination of gemcitabine-(C4-amide)-[anti-EGFR] with gemcitabine-(C4-amide)-[a
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| 篇名 | Simultaneous Dual Selective Targeted Delivery of Two Covalent Gemcitabine Immunochemotherapeutics and Complementary Anti-Neoplastic Potency of [Se]-Methylselenocysteine | ||
| 来源期刊 | 癌症治疗(英文) | 学科 | 医学 |
| 关键词 | GEMCITABINE ANTI-EGFR Anti-HER2/neu COVALENT Immunochemotherapeutic Gemcitabine-(C4-amide)-[Anti-EGFR] Gemcitabine-(C4-amide)-[Anti-HER2/neu] Mammary Adenocarcinoma (SKBr-3) [Se]-Methylselenocysteine | ||
| 年,卷(期) | 2015,(1) | 所属期刊栏目 | |
| 研究方向 | 页码范围 | 62-89 | |
| 页数 | 28页 | 分类号 | R73 |
| 字数 | 语种 | ||
| DOI | |||
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GEMCITABINE
ANTI-EGFR
Anti-HER2/neu
COVALENT
Immunochemotherapeutic
Gemcitabine-(C4-amide)-[Anti-EGFR]
Gemcitabine-(C4-amide)-[Anti-HER2/neu]
Mammary
Adenocarcinoma
(SKBr-3)
[Se]-Methylselenocysteine
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期刊影响力
癌症治疗(英文)
主办单位:
美国科研出版社
出版周期:
月刊
ISSN:
2151-1934
CN:
开本:
出版地:
武汉市江夏区汤逊湖北路38号光谷总部空间
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606
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0
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0
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