The COOH-terminal peptide of platelet factor-4 variant (CXCL4L1/PF-4var47-70) strongly inhibits angiogenesis and suppresses B16 melanoma growth in vivo.

Vandercappellen J; Liekens S; Bronckaers A; Noppen S; Ronsse I; Dillen C; Belleri M; Mitola S; Proost P; Presta M; Struyf S; Van Damme J

首页> 外文期刊>Molecular cancer research: MCR >The COOH-terminal peptide of platelet factor-4 variant (CXCL4L1/PF-4var47-70) strongly inhibits angiogenesis and suppresses B16 melanoma growth in vivo.

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The COOH-terminal peptide of platelet factor-4 variant (CXCL4L1/PF-4var47-70) strongly inhibits angiogenesis and suppresses B16 melanoma growth in vivo.

机译：血小板因子4变体的COOH末端肽（CXCL4L1 / PF-4var47-70）在体内强烈抑制血管生成并抑制B16黑色素瘤生长。

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Chemokines influence tumor growth directly or indirectly via both angiogenesis and tumor-leukocyte interactions. Platelet factor-4 (CXCL4/PF-4), which is released from alpha-granules of activated platelets, is the first described angiostatic chemokine. Recently, it was found that the variant of CXCL4/PF-4 (CXCL4L1/PF-4var) could exert a more pronounced angiostatic and antitumoral effect than CXCL4/PF-4. However, the molecular mechanisms of the angiostatic activities of the PF-4 forms remain partially elusive. Here, we studied the biological properties of the chemically synthesized COOH-terminal peptides of CXCL4/PF-4 (CXCL4/PF-4(47-70)) and CXCL4L1/PF-4var (CXCL4L1/PF-4var(47-70)). Both PF-4 peptides lacked monocyte and lymphocyte chemotactic activity but equally well inhibited (25 nmol/L) endothelial cell motility and proliferation in the presence of a single stimulus (i.e., exogenous recombinant fibroblast growth factor-2). In contrast, when assayed in more complex angiogenesis test systems characterized by the presence of multiple mediators, including in vitro wound-healing (2.5 nmol/L versus 12.5 nmol/L), Matrigel (60 nmol/L versus 300 nmol/L), and chorioallantoic membrane assays, CXCL4L1/PF-4var(47-70) was found to be significantly (5-fold) more angiostatic than CXCL4/PF-4(47-70). In addition, low (7 microg total) doses of intratumoral CXCL4L1/PF-4var(47-70) inhibited B16 melanoma growth in mice more extensively than CXCL4/PF-4(47-70). This antitumoral activity was predominantly mediated through inhibition of angiogenesis (without affecting blood vessel stability) and induction of apoptosis, as evidenced by immunohistochemical and fluorescent staining of B16 tumor tissue. In conclusion, CXCL4L1/PF-4var(47-70) is a potent antitumoral and antiangiogenic peptide. These results may represent the basis for the design of CXCL4L1/PF-4var COOH-terminal-derived peptidomimetic anticancer drugs.

机译：趋化因子通过血管生成和肿瘤-白细胞相互作用直接或间接影响肿瘤的生长。从活化血小板的α-颗粒释放的血小板因子4（CXCL4 / PF-4）是最早描述的血管抑制趋化因子。最近，发现CXCL4 / PF-4的变体（CXCL4L1 / PF-4var）比CXCL4 / PF-4具有更明显的血管抑制作用和抗肿瘤作用。但是，PF-4形式的血管抑制活性的分子机制仍然部分难以捉摸。在这里，我们研究了化学合成的CXCL4 / PF-4（CXCL4 / PF-4（47-70））和CXCL4L1 / PF-4var（CXCL4L1 / PF-4var（47-70））。两种PF-4肽都缺乏单核细胞和淋巴细胞的趋化活性，但是在单个刺激（即外源重组成纤维细胞生长因子2）存在下，内皮细胞的运动性和增殖同样受到抑制（25 nmol / L）。相反，在以多种介体为特征的更复杂的血管生成测试系统中进行分析时，包括体外伤口愈合（2.5 nmol / L与12.5 nmol / L），Matrigel（60 nmol / L与300 nmol / L），和绒膜尿囊膜测定，发现CXCL4L1 / PF-4var（47-70）的血管抑制作用比CXCL4 / PF-4（47-70）明显高（5倍）。此外，低剂量（总共7微克）的肿瘤内CXCL4L1 / PF-4var（47-70）比CXCL4 / PF-4（47-70）更广泛地抑制了小鼠的B16黑色素瘤生长。这种抗肿瘤活性主要是通过抑制血管生成（不影响血管稳定性）和诱导细胞凋亡来介导的，如B16肿瘤组织的免疫组织化学和荧光染色所证明。总之，CXCL4L1 / PF-4var（47-70）是一种有效的抗肿瘤和抗血管生成肽。这些结果可能代表了设计CXCL4L1 / PF-4var COOH-末端衍生的拟肽抗癌药物的基础。

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《Molecular cancer research: MCR》 |2010年第3期|共13页
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Vandercappellen J; Liekens S; Bronckaers A; Noppen S; Ronsse I; Dillen C; Belleri M; Mitola S; Proost P; Presta M; Struyf S; Van Damme J;
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1. Angiostatin基因真核表达载体的构建及对B16黑色素瘤体内生长抑制作用 [J] . 王季石, 孙等军, 郭礼和, 分子细胞生物学报（英文版） . 2002,第004期
2. The COOH-terminal peptide of platelet factor-4 variant (CXCL4L1/PF-4var47-70) strongly inhibits angiogenesis and suppresses B16 melanoma growth in vivo. [J] . Vandercappellen J, Liekens S, Bronckaers A, Molecular cancer research: MCR . 2010,第3期

机译：血小板因子4变体的COOH末端肽（CXCL4L1 / PF-4var47-70）在体内强烈抑制血管生成并抑制B16黑色素瘤生长。
3. The Chemokine Platelet Factor-4 Variant (PF-4var)/CXCL4L1 Inhibits Diabetes-Induced Blood-Retinal Barrier Breakdown [J] . Abu El-Asrar Ahmed M., Mohammad Ghulam, Nawaz Mohd Imtiaz, Investigative ophthalmology & visual science . 2015,第3期

机译：趋化因子血小板因子4变异体（PF-4var）/ CXCL4L1抑制糖尿病诱导的血视网膜屏障破坏。
4. Angiostatic and chemotactic activities of the CXC chemokine CXCL4L1 (platelet factor-4 variant) are mediated by CXCR3. [J] . Struyf S, Salogni L, Burdick MD, Blood: The Journal of the American Society of Hematology . 2011,第2期

机译：CXC趋化因子CXCL4L1（血小板因子4变体）的血管抑制和趋化活性由CXCR3介导。
5. α_vβ_3 INTEGRIN-TARGETED LIPOSOMES CONTAINING DOXORUBICIN INHIBIT TUMOR GROWTH AND ANGIOGENESIS IN A SYNGENEIC MURINE MELANOMA MODEL [C] . Charles A. Wartchow, Neal E. DeChene, S. Narasimhan Danthi, Proceedings of the 29th Annual Meeting of the Controlled Release Society . 2002

机译：含阿霉素抑制肿瘤生长和血管生成的α_vβ_3整合素靶向脂质体在共性鼠黑素瘤模型中的应用
6. The Chemokine Platelet Factor-4 Variant (PF-4var)/CXCL4L1 Inhibits Diabetes-Induced Blood–Retinal Barrier Breakdown [O] . Ahmed M. Abu El-Asrar, Ghulam Mohammad, Mohd Imtiaz Nawaz, -1

机译：趋化因子血小板因子4变异体（PF-4var）/ CXCL4L1抑制糖尿病诱导的血液-视网膜屏障破坏
7. The COOH-Terminal Peptide of Platelet Factor-4 Variant (CXCL4L1/PF-4var47-70) Strongly Inhibits Angiogenesis and Suppresses B16 Melanoma Growth In vivo. [O] . J. Vandercappellen, S. Liekens, A. Bronckaers, 2010

机译：血小板因子4变体的COOH末端肽（CXCL4L1 / PF-4var47-70）强烈抑制血管生成并抑制体内B16黑色素瘤的生长。

The COOH-terminal peptide of platelet factor-4 variant (CXCL4L1/PF-4var47-70) strongly inhibits angiogenesis and suppresses B16 melanoma growth in vivo.

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