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B16 melanoma tumor growth is delayed in mice in an age-dependent manner

机译:B16黑色素瘤肿瘤的生长以年龄依赖性方式延迟

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A major risk factor for cancer is increasing age, which suggests that syngeneic tumor implants in old mice would grow more rapidly. However, various reports have suggested that old mice are not as permissive to implanted tumor cells as young mice. In order to determine and characterize the age-related response to B16 melanoma, we implanted 5×105 tumor cells into 8, 16, 24, and 32-month-old male C57BL/6 (B6) and C57BL/6×BALB/c F1 (CB6 F1) mice subcutaneously in the inguinal and axillary spaces, or intradermally in the lateral flank. Results showed decreased tumor volume with increasing age, which varied according to mouse genetic background and the implanted site. The B6 strain showed robust tumor growth at 8 months of age at the inguinal implantation site, with an average tumor volume of 1341.25 mm3. The 16, 24, and 32-month age groups showed a decrease in tumor growth with tumor volumes of 563.69, 481.02, and 264.55 mm3, respectively (p≤0.001). The axillary implantation site was less permissive in 8-month-old B6 mice with an average tumor volume of 761.52 mm3. The 24- and 32-month age groups showed a similar decrease in tumor growth with tumor volumes of 440 and 178.19 mm3, respectively (p≤0.01). The CB6F1 strain was not as tumor permissive at 8 months of age as B6 mice with average tumor volumes of 446.96 and 426.91 mm3 for the inguinal and axillary sites, respectively. There was a decrease in tumor growth at 24 months of age at both inguinal and axillary sites with an average tumor volume of 271.02 and 249.12 mm3, respectively (p≤0.05). The strain dependence was not apparent in 8-month-old mice injected intradermally with B16 melanoma cells, with average tumor volumes of 736.82 and 842.85 mm3 for B6 and CB6 F1, respectively. However, a strain difference was seen in 32-month-old B6 mice with an average decrease in tumor volume of 250.83 mm3 (p≤0.01). In contrast, tumor growth significantly decreased earlier in CB6 F1 mice with average tumor volumes of 417.62 and 216.34 mm3 in the 16- and 24-month age groups, respectively (p≤0.005). Histologically, implanted tumors in young mice exhibited characteristics of aggressive, rapidly growing tumor cells including high vascularity, mitosis, and invasiveness compared to tumors in old mice. We contend that the decrease in B16 melanoma tumor growth seen with increasing age in B6 and CB6 F1 mice represents a biological process, which we are calling age-dependent cancer resistance (ADCR). Our data provide a detailed description of conditions necessary to use the model to investigate the mechanisms of ADCR and determine its biological and clinical relevance.
机译:癌症的主要危险因素是年龄增长,这表明老年小鼠的同基因肿瘤植入物将生长更快。然而,各种报道表明,年老的老鼠不像年幼的老鼠那样允许植入肿瘤细胞。为了确定和表征与年龄相关的对B16黑色素瘤的反应,我们将5×105肿瘤细胞植入8、16、24和32个月大的男性C57BL / 6(B6)和C57BL / 6×BALB / c F1(CB6 F1)小鼠在腹股沟和腋窝皮下或皮下外侧翼中。结果显示,随着年龄的增长,肿瘤体积减小,这取决于小鼠的遗传背景和植入部位。 B6菌株在腹股沟植入位点显示8个月大时肿瘤生长强劲,平均肿瘤体积为1341.25 mm3。 16、24和32个月大的年龄组显示肿瘤生长下降,肿瘤体积分别为563.69、481.02和264.55 mm3(p≤0.001)。在8个月大的B6小鼠中,腋窝植入位点的允许性较低,平均肿瘤体积为761.52 mm3。 24和32个月大的年龄组显示出相似的肿瘤生长下降,肿瘤体积分别为440和178.19 mm3(p≤0.01)。 CB6F1菌株在8个月大时不像B6小鼠那样具有良好的肿瘤容许性,腹股沟和腋窝部位的平均肿瘤体积分别为446.96和426.91 mm3。在腹股沟和腋窝部位,在24个月大时,肿瘤的生长均有所减少,平均肿瘤体积分别为271.02和249.12 mm3(p≤0.05)。在皮内注射B16黑色素瘤细胞的8个月大小鼠中,应变依赖性不明显,B6和CB6 F1的平均肿瘤体积分别为736.82和842.85 mm3。但是,在32个月大的B6小鼠中观察到了品系差异,肿瘤体积平均减少了250.83 mm3(p≤0.01)。相反,在CB6 F1小鼠中,肿瘤生长显着下降较早,在16和24个月龄组中平均肿瘤体积分别为417.62和216.34 mm3(p≤0.005)。从组织学上讲,与老年小鼠相比,在年轻小鼠中植入的肿瘤表现出侵袭性,快速生长的肿瘤细胞的特征,包括高血管,有丝分裂和侵袭性。我们认为,随着B6和CB6 F1小鼠年龄的增长,B16黑色素瘤肿瘤生长的减少代表了生物学过程,我们称其为年龄依赖性抗癌性(ADCR)。我们的数据提供了使用模型研究ADCR的机制并确定其生物学和临床相关性所需条件的详细描述。

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