Akasov Roman, Haq Sabah, Haxho Fiona, Samuel Vanessa, Burov Sergey V, Markvicheva Elena, Neufeld Ronald J, Szewczuk Myron R
Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, 117997 Moscow, Russia.
Department of Biomedical and Molecular Sciences, Queen's University, Kingston, Ontario, K7L 3N6 Canada.
Oncotarget. 2016 Oct 4;7(40):66119-66134. doi: 10.18632/oncotarget.11868.
Multicellular tumor spheroids (MTS) have been at the forefront of cancer research, designed to mimic tumor-like developmental patterns in vitro. Tumor growth in vivo is highly influenced by aberrant cell surface-specific sialoglycan structures on glycoproteins. Aberrant sialoglycan patterns that facilitate MTS formation are not well defined. Matrix-free spheroids from breast MCF-7 and pancreatic PANC1 cancer cell lines and their respective tamoxifen (TMX) and gemcitabine (Gem) resistant variants were generated using the RGD platform of cyclic Arg-Gly-Asp-D-Phe-Lys peptide modified with 4-carboxybutyl-triphenylphosphonium bromide (cyclo-RGDfK (TPP)). MCF-7 and MCF-7 TMX cells formed tight spheroids both in the classical agarose-and RGD-based platforms while all PANC1 cells formed loose aggregates. Using lectin histochemistry staining, sialidase assay, neuraminidase (Vibrio cholerae) and oseltamivir phosphate (OP) neuraminidase inhibitor treatments, MCF-7 and PANC1 cells and their drug-resistant variants expressed different sialic acid (SA) content on their cell surfaces. α-2,3- and α-2,6-sialic acid surface residues facilitated spheroid formation under cyclo-RGDfK(TPP)-induced self-assembly. Pretreatment with α-2,3- SA specific Maackia amurensis (MAL-II) lectin, α-2,6-SA specific Sambucus nigra (SNA) lectin, and exogenous α-2,6-SA specific neuraminidase (Vibrio cholerae) dose-dependently reduced spheroid volume. OP enhanced cell aggregation and compaction forming spheroids. PANC1 and MDA-MB231 xenograft tumors from untreated and OP-treated RAGxCγ double mutant mice expressed significantly higher levels of α-2,3- SA over α-2,6-SA. MCF-7 spheroids also expressed a high α-2,3-SA to α-2,6-SA ratio. These results suggest that the relative levels of specific sialoglycan structures on the cell surface correlate with the ability of cancer cells to form avascular multicellular tumor spheroids and in vivo xenograft tumors.
多细胞肿瘤球体(MTS)一直处于癌症研究的前沿,旨在体外模拟肿瘤样发育模式。体内肿瘤生长受到糖蛋白上异常细胞表面特异性唾液酸聚糖结构的高度影响。促进MTS形成的异常唾液酸聚糖模式尚未明确界定。使用用4-羧基丁基三苯基溴化膦修饰的环状精氨酸-甘氨酸-天冬氨酸-D-苯丙氨酸-赖氨酸肽(环RGDfK(TPP))的RGD平台,从乳腺癌MCF-7和胰腺PANC1癌细胞系及其各自的他莫昔芬(TMX)和吉西他滨(Gem)耐药变体中生成无基质球体。MCF-7和MCF-7 TMX细胞在经典的基于琼脂糖和基于RGD的平台中均形成紧密的球体,而所有PANC1细胞均形成松散的聚集体。使用凝集素组织化学染色、唾液酸酶测定、神经氨酸酶(霍乱弧菌)和磷酸奥司他韦(OP)神经氨酸酶抑制剂处理,MCF-7和PANC1细胞及其耐药变体在其细胞表面表达不同的唾液酸(SA)含量。α-2,3-和α-2,6-唾液酸表面残基在环RGDfK(TPP)诱导的自组装下促进球体形成。用α-2,3-SA特异性的黑果接骨木(MAL-II)凝集素、α-2,6-SA特异性的黑接骨木(SNA)凝集素和外源性α-2,6-SA特异性神经氨酸酶(霍乱弧菌)进行预处理,剂量依赖性地减小了球体体积。OP增强细胞聚集并压实形成球体。来自未处理和OP处理的RAGxCγ双突变小鼠的PANC1和MDA-MB231异种移植肿瘤表达的α-2,3-SA水平明显高于α-2,6-SA。MCF-7球体也表达高的α-2,3-SA与α-2,6-SA比率。这些结果表明,细胞表面特定唾液酸聚糖结构的相对水平与癌细胞形成无血管多细胞肿瘤球体和体内异种移植肿瘤的能力相关。
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