日韩黄色在线 中文字幕-国产亚洲99久久精品免费-99热久这里只有精品-9丨精品人妻一区二区三区密桃-成人免费黄色大片v266-17c久久精品国产亚洲av蜜柚-精品久久久免费观看-丰满人妻少妇一区二区三区-中文字幕欧美日韩制服,91麻豆精品91久久久久,欧美一区二区三区不卡高清视,99re国内精品视频

技術文章您現(xiàn)在的位置:首頁 > 技術文章 > 氯膦酸鹽脂質體介導的腫瘤相關巨噬細胞(TAM)耗竭:一種新的高效抗血管生成治療方法

氯膦酸鹽脂質體介導的腫瘤相關巨噬細胞(TAM)耗竭:一種新的高效抗血管生成治療方法

更新時間:2024-11-21   點擊次數(shù):1571次

中文摘要:

腫瘤相關巨噬細胞 (TAM) 通過促進腫瘤血管生成在腫瘤生長和轉移中起關鍵作用。用包埋在脂質體中的氯膦酸鹽 (Clodronate Liposomes) 治療有效地耗盡了小鼠 F9 畸胎癌和人 A673 橫紋肌肉瘤小鼠腫瘤模型中的這些吞噬細胞,導致腫瘤生長的顯著抑制,范圍為 75% 至 >92%,具體取決于治療和時間表。腫瘤抑制伴隨著腫瘤組織中血管密度的急劇降低。血管內皮生長因子 (VEGF) 是腫瘤血管生成的主要誘導劑之一,也是巨噬細胞募集所必需的。氯膦鹽脂質體和 VEGF 中和抗體的聯(lián)合治療觀察到效為優(yōu),而游離氯膦酸鹽沒有顯著活性。腫瘤的免疫組織學評估顯示 F4/80+ 和 MOMA-1+ 顯著耗竭,而 CD11b+ TAM 耗竭不太明顯。A673 模型中血管染色 (CD31) 和血管以及 TAM 和腫瘤相關樹突狀細胞 (TADC) 的定量顯示,即使在治療結束后 9 天,復位率也為 85% 至 >94%。此外,CD11c+ TADC 已被證明在腫瘤釋放的生長和分化因子刺激后可能分化為內皮樣細胞,氯膦鹽脂質體或抗體治療同樣降低了 CD11c+ TADC。這些結果驗證了氯膦酸鹽脂質體 (Clodronate Liposomes) 療法與血管生成抑制劑聯(lián)合使用是一種很有前途的新型癌癥治療策略,用于針對刺激腫瘤生長和播散的造血前體細胞,并作為研究巨噬細胞和樹突狀細胞在腫瘤發(fā)生中的作用的工具。

英文摘要:

Tumour-associated macrophages, TAMs, play a pivotal role in tumour growth and metastasis by promoting tumour angiogenesis. Treatment with clodronate encapsulated in liposomes (clodrolip) efficiently depleted these phagocytic cells in the murine F9 teratocarcinoma and human A673 rhabdomyosarcoma mouse tumour models resulting in significant inhibition of tumour growth ranging from 75 to >92%, depending on therapy and schedule. Tumour inhibition was accompanied by a drastic reduction in blood vessel density in the tumour tissue. Vascular endothelial growth factor (VEGF) is one of the major inducers of tumour angiogenesis and is also required for macrophage recruitment. The strongest effects were observed with the combination therapy of clodrolip and a VEGF-neutralising antibody, whereas free clodronate was not significantly active. Immunohistologic evaluation of the tumours showed significant depletion of F4/80+ and MOMA-1+ and a less pronounced depletion of CD11b+ TAMs. Blood vessel staining (CD31) and quantification of the vessels as well as TAMs and tumour-associated dendritic cells (TADCs) in the A673 model showed reduction rates of 85 to >94%, even 9 days after the end of therapy. In addition, CD11c+ TADCs, which have been shown to potentially differentiate into endothelial-like cells upon stimulation by tumour released growth and differentiation factors, were similarly reduced by clodrolip or antibody treatment. These results validate clodrolip therapy in combination with angiogenesis inhibitors as a promising novel strategy for an indirect cancer therapy aimed at the haematopoietic precursor cells that stimulate tumour growth and dissemination and as a tool to study the role of macrophages and dendritic cells in tumorigenesis.


論文信息:

論文題目: Clodronate-liposome-mediated depletion of tumour-associated macrophages: a new and highly effective antiangiogenic therapy approach

期刊名稱:British Journal of Cancer

時間期卷: volume 95, pages272–281 (2006)

在線時間:2006年7月11日

DOI: doi.org/10.1038/sj.bjc.6603240


Liposoma巨噬細胞清除劑氯膦酸鹽脂質體Clodronate Liposomes見刊于BJC:

氯膦酸鹽脂質體介導的腫瘤相關巨噬細胞(TAM)耗竭:一種新的高效抗血管生成治療方法


Liposoma巨噬細胞清除劑氯膦酸鹽脂質體Clodronate Liposomes的材料和方法

氯膦酸鹽脂質體介導的腫瘤相關巨噬細胞(TAM)耗竭:一種新的高效抗血管生成治療方法

氯膦酸鹽脂質體介導的腫瘤相關巨噬細胞(TAM)耗竭:一種新的高效抗血管生成治療方法,巨噬細胞清除解決方案

Tumour models and therapies-體內實驗

Exponentially growing F9 teratocarcinoma (7 × 106?50?μl?1) or A673 rhabdomyosarcoma cells (6–8 × 106?50?μl?1 mixed 1?:?1, v?v?1 with Matrigel, Beckton Dickinson, Basel, Switzerland) were injected subcoutanously (s.c.) on the flanks of mice. Treatment was started 6?h after inoculation of F9 cells (female Sv129 mice) and 24?h after inoculation of A673 cells (female CD-1 nude mice), respectively. The mice (6–8/group) received clodronate dissolved in phosphate buffer (PB, 67?mM, pH 7.4) or clodrolip by intraperitoneal (i.p.) injection as initial dose of 2?mg?20?g?1 mouse body weight, followed by 1?mg for the subsequent doses. The Abs were given at 0.5?mg?20?g?1 mouse body weight in 100?μl PB by intravenous (i.v.) injection into the tail vein. Tumour growth was measured in a blinded fashion with a caliper and volumes were calculated using the equation: V=πab2/6 (a=largest tumour diameter, b=perpendicular diameter). Relative percentual tumour growth was normalised to day one. Mice were killed 8–22 days after onset of treatment and tumours and spleens removed for histology.

6-8周,20g小鼠,首劑量腹腔注射2mg,按Liposoma產品貨號CP-005-005,規(guī)格是5ml+5ml。濃度是5mg/ml。相當于注射了400ul,后期是1mg劑量維持,也就是注射200ul。

Cytotoxicity assay-體外實驗

The in vitro cytotoxicity of clodronate was assessed as described before . Briefly, cells were incubated in 96-well plates with liposomes, clodronate and clodrolip (6?h, 37°C, 1?mg clodronate?ml?1) and cell viability was determined by addition of WST-1 reagent (Roche Diagnostics, Mannheim, Germany) according to the manufacturer's recommendations.


靶點科技(北京)有限公司

靶點科技(北京)有限公司

地址:中關村生命科學園北清創(chuàng)意園2-4樓2層

© 2026 版權所有:靶點科技(北京)有限公司  備案號:京ICP備18027329號-2  總訪問量:385710  站點地圖  技術支持:化工儀器網(wǎng)  管理登陸

欧美亚洲国产日韩成人在线-欧美黑人激情精品在线-精品久久久久久久久久久久久蜜桃-91福利色免费观看 | 干日本女人大逼-欧美日韩一级a在线观看-超碰免费在线公开精品-人妻有码av中文字幕久久琪 | 亚洲精品乱码久久-人人妻人人澡人人爽精品日本-精品人妻少妇久久久久久久久久久-欧美经典一区二区三区视频 | 五月婷婷丁香婷婷爱爱-婷婷激情久久成人网-天天操天天草天天干天天日-欧美日韩一区二区一卡二卡 超碰免费在线97资源-99热在线视频观看免费-久久久久人妻一区精品免费看-超碰免费人妻中文 | 91久久婷婷国产麻豆精品电影视频-久久国产v一级毛多内射-国产精品 欧美在线-欧美日韩一区二区三区图片 | 婷婷久久久一区二区-欧美高清一区二区三区不卡视频-久久伊人网亚洲精品-在线人妻久久中文字幕 | 精品 一区二区三区四区-国产成人户外露出视频在线观看-国产精品麻豆密视频-婷婷激情六月天亚洲区 | 亚洲乱码精品久久久久久..-最近最好的中文字幕免费-99精品乱码久久久久-精品国产亚洲精品1 | 中文字幕亚洲精品乱码-高清不卡二卡三卡四卡无卡-国产综合一区二区三区av-69精品久久久久久久久久久久 | 国产精品精品麻豆-日韩亚洲丝袜系列-999个精品小视频-久久久久久久91精品 | 99精品网站视频在线观看-久久99精品视频推荐-日韩av在线电影免费看-精品丝袜美腿中文字幕 | 亚洲va欧美va人人爽2-中文字幕人妻少妇精品-91超碰国产熟女嗷嗷-欧美午夜精品久久久久久免费 | 热re99国产精品66热-婷婷六月色综合国产-国产精品久久高潮呻吟av-日韩午夜免费av | 久久99精品视频.-超碰 天天干 天天摸-欧美人妻伦理中文字幕在线-黑人操日本美女 | shkd697脱狱者中文字幕-久久王色禄象视频免-我的美女丝袜人妻中文字幕-色婷婷狠狠禁久久yy | 日韩激情文字在线-人妻中文字幕蜜桃av-亚洲激情人妻av-日韩伦理高清在线视频 | 91超精品碰国产在线观看-91人精品久久久久久久久-日韩老熟妇精品-久久在线视频首页 | 久久久激情婷婷丁香激情-精品日本一区二区三区视频播放-久久精品国产精品久久-人妻系列中出中文字幕一区二区 | 麻豆黄片在线观看-日韩日韩日韩日韩日韩熟女-中文字幕精品熟女人妻-69精品人妻久久久久久久 | 久久99免费福利视频-色婷婷综合久久久久中文一区二-国产久久久9999-人妻熟女中文字幕一区二区 | 成人欧美日韩一区二区三区-国产亚洲欧美日韩视频-热re99久久精品国产首页日韩-日本在线中文字幕一区二区 | 99精品免费公开视频-国产精品久久av呻吟-日韩伦理在线视频中文字幕-国产美女久久久av | 丁香花视频在线观看完整版中文-色婷婷久久综合久色综合8-超碰福利免费人妻-9999久久久久久 | 91人妻精品久久久久久久久熟妇-91精品久久久老熟女9久-隔壁人妻 中文字幕-成人大香蕉一区二区三区 | shkd697脱狱者中文字幕-久久王色禄象视频免-我的美女丝袜人妻中文字幕-色婷婷狠狠禁久久yy | 精品久久久久久久高清-日韩一区二区黄色片-日本中文字幕有码电影在线观看-久久久久久久久四区三区 | 人妻精品免费一区二区三区四区-日韩亚洲欧美在线第一-国产精品永久免费99久久-日韩三级四级成人黄色 | 97在线观看视频免费观看-高清欧美性猛xxxx黑人猛交-久久人妻精品大奶一区二区-日韩人妻少妇精品中文字幕 | 国产成人大片在线观看-熟妇人妻中文字幕在线视频-久久精品一区二区三区四区-欧美精品久久99久久 beeg老熟妇喷水-av黄色一级片在线观看第二区-亚洲av日韩综合一区在线观看-婷婷www久久 | 日韩av在线视频播放-婷婷国产免费视频久久-18禁国产精品久久久久久久久久-97人妻人人澡人人爽人国产网址 | 热久久色播激情-久久婷婷sese-国产精品v高清不卡a久久-久久久熟妇熟女av | 日韩激情文字在线-人妻中文字幕蜜桃av-亚洲激情人妻av-日韩伦理高清在线视频 | 日韩中文字幕a欧美v-国产69精品久久久久999天美-人妻熟女,日韩有码-久久免费看女人 | 人妻精品免费一区二区三区四区-日韩亚洲欧美在线第一-国产精品永久免费99久久-日韩三级四级成人黄色 | 中文字幕亚洲精品乱码-高清不卡二卡三卡四卡无卡-国产综合一区二区三区av-69精品久久久久久久久久久久 | 蜜桃一区二区人妻熟女-99日韩人妻一区二区三区合部-日韩视频免费观看一区-欧美日韩中文字幕在线观看视频 | 久久久艹大香蕉伊人网-无套内射高清在线-日韩最新av在线-国产99免费手机在线视频 | 日本在线一区二区不卡视频-www亚洲精品久久久乳-国产精品人妻熟女av久久夜色-国产自拍激情视频在线观看 | 国产一精品一av一免费爽爽-色婷婷午夜激情av-精品人妻一区二区三区网站-超碰人人妻人人爽最新 | 国产精品又粗又猛又爽又黄-91福利久久福利精品-日韩人妻在线中文字幕在线视频-亚洲口爆深喉在线观看 | 国产精品又粗又猛又爽又黄-91福利久久福利精品-日韩人妻在线中文字幕在线视频-亚洲口爆深喉在线观看 |