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消炎痛对兔VX2癌所致前列腺素、破骨细胞及骨破坏的控制时机

Timing of indomethacin in the control of prostaglandins, osteoclasts and bone destruction produced by VX2 carcinoma in rabbits.

作者信息

Galasko C S, Rawlins R, Bennett A

出版信息

Br J Cancer. 1979 Sep;40(3):360-4. doi: 10.1038/bjc.1979.189.

Abstract

Rabbits were injected with VX2 cancer cells into the left thigh or tibia, and given indomethacin 1-16 mg/kg daily starting on the day before tumour implantation or 7, 14 or 21 days after implantation. Indomethacin at 2 mg/kg and above from before tumour implantation reduced osteoclast proliferation and the amount of prostaglandin-like material extracted from homogenates of excised tumours, but the inhibition of bone destruction in vivo was significant only with indomethacin at 4 mg/kg and above. Indomethacin at 8 mg/kg reduced osteoclast proliferation and bone destruction, but the effect was statistically significant only when given within 7 days of inoculation with the tumour. The place of indomethacin and other inhibitors of prostaglandin synthesis has not yet been established in the management of patients with skeletal metastases. Drug administration might need to be started at the time of diagnosis and removal of the primary tumour, rather than when skeletal metastases are evident.

摘要

将VX2癌细胞注射到兔子的左大腿或胫骨中,并从肿瘤植入前一天或植入后7、14或21天开始,每天给予1 - 16毫克/千克的吲哚美辛。从肿瘤植入前开始给予2毫克/千克及以上剂量的吲哚美辛,可减少破骨细胞增殖以及从切除肿瘤的匀浆中提取的前列腺素样物质的量,但仅4毫克/千克及以上剂量的吲哚美辛对体内骨破坏的抑制作用才显著。8毫克/千克的吲哚美辛可减少破骨细胞增殖和骨破坏,但仅在接种肿瘤后7天内给药时,其效果才有统计学意义。吲哚美辛和其他前列腺素合成抑制剂在骨骼转移患者的治疗中的地位尚未确立。给药可能需要在诊断和切除原发性肿瘤时开始,而不是在骨骼转移明显时开始。

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本文引用的文献

1
Extraction of prostaglandins from human blood.从人体血液中提取前列腺素。
Nature. 1971 Oct 1;233(5318):336-7. doi: 10.1038/233336b0.
3
Prostaglandin production and bone resorption by dental cysts.
Nature. 1973 Sep 28;245(5422):213-5. doi: 10.1038/245213a0.
4
Prostaglandin E2 and gastric acid secretion in man.前列腺素E2与人体胃酸分泌
J Physiol. 1973 Mar;229(2):349-60. doi: 10.1113/jphysiol.1973.sp010142.
9
Prostaglandins and breast cancer.前列腺素与乳腺癌
Lancet. 1977 Sep 24;2(8039):624-6. doi: 10.1016/s0140-6736(77)92496-5.

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