贝伐单抗给药后,血浆和血清中VEGF - A121的浓度升高,而VEGF - A165的浓度未升高。
Plasma and serum concentrations of VEGF-A121, but not of VEGF-A165, increase post-bevacizumab administration.
作者信息
Okawa Masashi, Yamakuchi Munekazu, Bibek Aryal, Takenouchi Kazunori, Maywar Drew N, Yamada Shingo, Inoue Keiichi, Higurashi Kazuhiko, Nakazawa Junichi, Kawahira Masahiro, Kodama Tomoko, Tanoue Kiyonori, Oyama Yoko, Higashi Sadayuki, Fujisaki Chieko, Hashinokuchi Hirohito, Tabaru Akito, Kanda Hideaki, Tachioka Shuji, Imoto Yutaka, Hashiguchi Teruto, Soga Yoshiharu
机构信息
Department of Cardiovascular and Gastroenterological Surgery, Graduate School of Medical and Dental Sciences, Kagoshima University, Kagoshima, Japan.
Department of Laboratory and Vascular Medicine, Graduate School of Medical and Dental Sciences, Kagoshima University, Kagoshima, Japan.
出版信息
PLoS One. 2024 Dec 19;19(12):e0316035. doi: 10.1371/journal.pone.0316035. eCollection 2024.
BACKGROUND
VEGF-A concentrations were measured in the blood of bevacizumab-treated cancer patients in previous studies, but a consensus has not formed that would develop VEGF-A into a clinical biomarker. Recently, methods to strictly distinguish between the VEGF-A isoforms have been developed but have not yet been applied to cancer patients undergoing bevacizumab treatment.
METHODS
An ELISA that strictly distinguishes between VEGF-A121 and VEGF-A165-the major isoforms of VEGF-A-and a commercially available ELISA for VEGF-A are used to determine the concentration of VEGF-A121, VEGF-A165, and VEGF-A in the blood of 12 patients with advanced colorectal cancer receiving bevacizumab therapy.
RESULTS
The serum and plasma concentrations of VEGF-A121 increased substantially post-bevacizumab administration; the median increase in serum was 860.8 pg/mL, 95% confidence interval (CI) [468.5, 1128.9], p = 0.0024, and in plasma was 808.6 pg/mL, 95% CI [748.7, 874.0], p = 0.00049. In stark contrast, VEGF-A165 after bevacizumab administration decreased in serum by a medium change of -73.8 pg/mL, 95% CI [-149.4, -10.2], p = 0.0034, with 83.3% of the post-bevacizumab concentrations falling below the high-accuracy threshold of 38 pg/mL; in plasma, all pre and post VEGF-A165 concentrations fell below this threshold. Concentrations of VEGF-A121 and VEGF-A165 in platelets did not change to a statistically significant degree. Adding recombinant VEGF-A121 (and -A165) or bevacizumab to plasma in patients post-bevacizumab administration increased or decreased, respectively, VEGF-A121 and VEGF-A165 levels. The increase in VEGF-A121 in plasma and serum after bevacizumab administration may be due to the dissociation of the complex of tumor-derived VEGF-A121 and bevacizumab when it moves from the stroma into the blood.
CONCLUSIONS
The VEGF-A121 isoform has been uniquely demonstrated as a clear marker of bevacizumab therapy in both plasma and serum, motivating further research on pursuing these isoforms as biomarkers in cancer care.
背景
在先前的研究中,已对接受贝伐单抗治疗的癌症患者血液中的VEGF - A浓度进行了测量,但尚未形成将VEGF - A开发为临床生物标志物的共识。最近,已开发出严格区分VEGF - A亚型的方法,但尚未应用于接受贝伐单抗治疗的癌症患者。
方法
使用一种能严格区分VEGF - A的主要亚型VEGF - A121和VEGF - A165的酶联免疫吸附测定(ELISA)以及一种市售的VEGF - A ELISA,来测定12例接受贝伐单抗治疗的晚期结直肠癌患者血液中VEGF - A121、VEGF - A165和VEGF - A的浓度。
结果
贝伐单抗给药后,VEGF - A121的血清和血浆浓度大幅增加;血清中值增加860.8 pg/mL,95%置信区间(CI)[468.5, 1128.9],p = 0.0024,血浆中值增加808.6 pg/mL,95% CI [748.7, 874.0],p = 0.00049。与之形成鲜明对比的是,贝伐单抗给药后,血清中VEGF - A165降低,中值变化为 - 73.8 pg/mL,95% CI [-149.4, -10.2],p = 0.0034,83.3%的贝伐单抗给药后浓度低于38 pg/mL的高精度阈值;在血浆中,VEGF - A165给药前和给药后的所有浓度均低于该阈值。血小板中VEGF - A121和VEGF - A165的浓度变化无统计学意义。在贝伐单抗给药后的患者血浆中添加重组VEGF - A121(和 - A165)或贝伐单抗分别增加或降低了VEGF - A121和VEGF - A165水平。贝伐单抗给药后血浆和血清中VEGF - A121的增加可能是由于肿瘤来源的VEGF - A121与贝伐单抗的复合物从基质进入血液时发生解离。
结论
VEGF - A121亚型已被独特地证明是血浆和血清中贝伐单抗治疗的明确标志物,这激发了进一步研究将这些亚型作为癌症治疗生物标志物的动力。
Zotero 插件