首页> 美国卫生研究院文献>British Journal of Cancer >Active melanogenesis in non-S phase melanocytes in B16 melanomas in vivo investigated by double-tracer microautoradiography with 18F-fluorodopa and 3H-thymidine.
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Active melanogenesis in non-S phase melanocytes in B16 melanomas in vivo investigated by double-tracer microautoradiography with 18F-fluorodopa and 3H-thymidine.

机译:B16黑色素瘤体内非S期黑色素细胞的活跃黑色素生成通过双示踪微放射自显影术与18F-氟多巴和3H-胸苷共同研究。

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摘要

3,4-Dihydroxy-2-[18F]fluoro-L-phenylalanine (2-[18F]FDOPA) and [6-3H]thymidine ([3H]Thd) were simultaneously injected into mice transplanted with B16 melanomas of FM3A mammary carcinoma. Melanogenesis was differentiated from DNA synthesis in the mitotic cell cycle by monitoring grain distribution with double-tracer microautoradiography. The percentages of pigmented cells were inversely proportional to those of [3H]Thd-labelled cells, indicating that the greater the number of melanocytes, the smaller was the number of proliferating cells. The number of grains produced by 2-[18F]FDOPA in the [3H]Thd-unlabelled melanocytes was significantly higher (P < 0.001) than the numbers in the [3H]Thd-labelled melanocytes and in nonmelanocytes. The [3H]Thd-unlabelled non-melanocytes and FM3A cells showed the lowest accumulation of 2-[18F]DOPA, which may have resulted from the basic amino acid demand by malignant neoplasms via amino acid transport. The [3H]Thd-labelled cells, regardless of whether they were pigmented or not, had slightly more grains with 2-[18F]FDOPA than the [3H]Thd-unlabelled non-melanocytes (P < 0.05), which may have resulted from the enhanced amino acid requirement for proliferation. Melanogenesis appeared to be activated only in the non-S phase of the mitotic cycle in melanocytes.
机译:将3,4-二羟基-2- [18F]氟-L-苯丙氨酸(2- [18F] FDOPA)和[6-3H]胸苷([3H] Thd)同时注射到移植有FM3A乳腺癌B16黑色素瘤的小鼠中。黑色素生成与有丝分裂细胞周期中的DNA合成不同,这是通过使用双示踪微放射自显影技术监测颗粒分布来实现的。色素细胞的百分比与[3H] Thd标记的细胞的百分比成反比,表明黑色素细胞的数量越多,增殖细胞的数量越少。 2- [18F] FDOPA在未标记[3H] Thd的黑素细胞中产生的谷粒数量显着高于[3H] Thd标记的黑素细胞和非黑素细胞(P <0.001)。 [3H] Thd未标记的非黑素细胞和FM3A细胞显示2- [18F] DOPA的最低积累,这可能是由于恶性肿瘤通过氨基酸转运对碱性氨基酸的需求所致。 [3H] Thd标记的细胞,无论是否着色,与[3H] Thd标记的非黑素细胞相比,具有[[3H] Thd标记的非黑素细胞)的2- [18F] FDOPA晶粒略多(P <0.05)从增加的氨基酸需求增殖。黑色素生成似乎仅在黑色素细胞有丝分裂周期的非S期被激活。

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