1995
DOI: 10.1038/bjc.1995.227
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Variation of growth rate of a rat tumour during a light-dark cycle: correlation with circadian fluctuations in tumour blood flow

Abstract: Summary To determine whether tumour growth is influenced by circadian variations in tumour tissue blood flow, we measured changes in area doubling time of tumours (Sato lung carcinoma) within transparent chambers and changes in tissue blood flow of rat subcutaneous tumour during a light-dark cycle. Rats were subjected to an artificial light-dark cycle with light from 7 a.m. to 7 p.m. Tumour doubling times (TDTs) dunrng the dark and the light spans were 33.5 ± 11.9 h (n = 38, 20 rats) and 70.6 ± 36.9 h (n = 39,… Show more

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Cited by 28 publications
(23 citation statements)
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“…Following these beats, three sets of clock-controlled protein increase and decrease: WEE-1 gates tumor cell mitosis; TSA gates 5-FU sensitivity and therapeutic index; and VEGF, along with other clockcontrolled genes, coordinates cancer blood flow and growth (29,30). This work shows for the first time the more or less complete chain of events responsible for repeated experimental and clinical findings that time of day proliferation-targeted anticancer drug, such as 5-FU, is given, determines its therapeutic index (31 -33).…”
Section: Discussionmentioning
confidence: 99%
“…Following these beats, three sets of clock-controlled protein increase and decrease: WEE-1 gates tumor cell mitosis; TSA gates 5-FU sensitivity and therapeutic index; and VEGF, along with other clockcontrolled genes, coordinates cancer blood flow and growth (29,30). This work shows for the first time the more or less complete chain of events responsible for repeated experimental and clinical findings that time of day proliferation-targeted anticancer drug, such as 5-FU, is given, determines its therapeutic index (31 -33).…”
Section: Discussionmentioning
confidence: 99%
“…Although SLC and LY80 showed almost the same growth potential in the transparent chamber and showed almost the same reaction after AC7700 administration, we chose SLC rather than LY80 for vital microscopic observations. We did so because when SLC is growing in transparent chambers, demarcation between the edge of the growing tumour and the normal tissue is clear (Hori et al, 1995), and therefore the change in normal arterioles and tumour vessels after AC7700 administration can easily be recognised.…”
Section: Rats and Tumoursmentioning
confidence: 99%
“…and s.c. transplantations, respectively. We chose SLC for vital microscopic observations because when the tumour is implanted in transparent chambers, demarcation between the edge of the growing tumour and normal tissue is clear, and therefore the change in microtumour size after therapy can easily be measured (Hori et al, 1995). Experiments were performed with the animals anaesthetised in a controlled-temperature box fitted with a suction duct.…”
Section: Rats and Tumourmentioning
confidence: 99%