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Augmentation in Chemosensitivity of Intratumor Quiescent Cells by Combined Treatment with Nicotinamide and Mild Hyperthermia

机译:烟酰胺和轻度热疗联合治疗可增强肿瘤内静止细胞的化学敏感性

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摘要

C3H/He and Balb/c mice bearing SCC VII and EMT6/KU tumors, respectively, received continuous administration of 5‐bromo‐2′‐deoxyuridine (BrdU) for 5 days using implanted mini‐osmotic pumps to label all proliferating (P) cells. Nicotinamide was administered intraperitoneally before cisplatin injection and/or tumors were locally heated at 40°C for 60 min immediately after cisplatin injection. The tumors were then excised, minced and trypsinized. The tumor cell suspensions were incubated with cytochalasin‐B (a cytokinesis‐blocker), and the micronucleus (MN) frequency in cells without BrdU labeling (quiescent (Q) cells) was determined using immunofluorescence staining for BrdU. The MN frequency in total (P+Q) tumor cells was determined from tumors that had not been pretreated with BrdU labeling. The sensitivity to cisplatin was evaluated in terms of the frequency of induced micronuclei in binuclear tumor cells (MN frequency). In both tumor systems, the MN frequency in Q cells was lower than that in the total cell population. Nicotinamide treatment elevated the MN frequency in total SCC VII cells. Mild heating raised the MN frequency more markedly in Q cells than in total cells. The combination of nicotinamide and mild heat treatment increased the MN frequency more markedly than either treatment alone. In total SCC VII cells, nicotinamide increased 195mPt‐cisplatin uptake. Mild heating elevated 195mPt‐cisplatin uptake in total EMT6/KU cells. Cisplatin‐sensitivity of Q cells was lower than that of total cells in both tumor systems. Nicotinamide sensitized tumor cells including a large acutely hypoxic fraction, such as those of SCC VII tumors, through inhibition of the fluctuations in tumor blood flow. Tumor cells including a large chronically hypoxic fraction such as Q cells were thought to be sensitized by mild heating through an increase in tumor blood flow.
机译:分别携带SCC VII和EMT6 / KU肿瘤的C3H / He和Balb / c小鼠使用植入的微型渗透泵标记所有增生的(P)连续5溴2'-脱氧尿苷(BrdU)连续5天细胞。顺铂注射前腹膜内给予烟酰胺和/或在顺铂注射后立即将肿瘤在40°C局部加热60分钟。然后切除肿瘤,切碎并用胰蛋白酶消化。将肿瘤细胞悬液与细胞松弛素B(一种胞质分裂阻滞剂)一起孵育,并使用BrdU免疫荧光染色确定了未标记BrdU的细胞(静止(Q)细胞)中的微核(MN)频率。从尚未经过BrdU标记预处理的肿瘤中确定总(P + Q)肿瘤细胞的MN频率。根据双核肿瘤细胞中诱导的微核的频率(MN频率)评估对顺铂的敏感性。在两个肿瘤系统中,Q细胞的MN频率均低于总细胞群的MN频率。烟酰胺处理提高了总SCC VII细胞的MN频率。温和的加热使Q电池中的MN频率比总电池中的MN频率显着提高。烟酰胺和温和热处理的组合比单独使用任何一种处理更显着地增加了MN频率。在总的SCC VII细胞中,烟酰胺增加了 195m Pt-顺铂的摄取。轻度加热会增加EMT6 / KU细胞中 195m 铂对顺铂的摄取。在两个肿瘤系统中,Q细胞的顺铂敏感性均低于总细胞。通过抑制肿瘤血流的波动,烟酰胺致敏的肿瘤细胞包括较大的急性低氧部分,例如SCC VII肿瘤。包括大量慢性低氧部分的肿瘤细胞(例如Q细胞)被认为通过增加肿瘤血流量而受到温和加热而致敏。

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