Marker rhythmometry with macrophage-colony stimulating factor (M-CSF).

Chronobiologia Pub Date : 1991-10-01
S Elg, E Halberg, S Ramakrishnan, G Cornélissen, E Haus, G Nicolau, L Carson, L Twiggs, H J Long, F Halberg
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Abstract

In a patient with a debulked müllerian adenocarcinoma involving the ovary, an elevated serum concentration of macrophage-colony stimulating factor (M-CSF) (5.3 ng/ml) was lowered into the range of the age- and gender-matched controls by a 24-hour infusion of 135 mg/m2 of taxol, as was a Ca125 of 1480 U/ml by three such taxol courses given at 3-week intervals (to 14 U/ml). A downward trend of M-CSF in serum with an about-14-hour ultradian modulation during the first chemotherapy course resembles that of the concomitantly assessed Ca125. A decreasing trend modulated by an about-half-weekly component is found in M-CSF of fractionated urines collected at spontaneous voidings around the clock for 5 days. M-CSF may serve as a chronobiologic marker for optimizing, on an individualized basis, 1) the infradian scheduling of chemotherapy courses and 2) the ultradian-circadian within-course time patterns. Timing based on markers of the anticancer effect aims at teh as-yet unattained transfer from rodent to human of cancer cures that were not previously feasible without chronobiologic considerations. This goal can be pursued with M-CSF as well as Ca125 and UGP as possibly complementary chronobiologic markers in a chronotherapy trial with taxol in humans.

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巨噬细胞集落刺激因子(M-CSF)标记心律测定。
在一例累及卵巢的勒氏腺癌患者中,通过24小时输注135 mg/m2紫杉醇,将血清巨噬细胞集落刺激因子(M-CSF)升高的浓度(5.3 ng/ml)降低到与年龄和性别匹配的对照组的范围内,Ca125为1480 U/ml,通过3周间隔给予3个紫杉醇疗程(至14 U/ml)。在第一次化疗过程中,血清中M-CSF的下降趋势与同期评估的Ca125相似,并伴有约14小时的超昼夜调节。在连续5天的自然排空中收集的分馏尿液的M-CSF中发现了大约半周成分调节的下降趋势。M-CSF可以作为一种时间生物学标记物,在个体化的基础上,优化1)化疗疗程的短期计划和2)疗程内的超昼夜时间模式。基于抗癌作用标记物的时间安排旨在实现尚未实现的从啮齿动物到人类的癌症治疗转移,如果没有时间生物学的考虑,这在以前是不可实现的。在紫杉醇的人体时间治疗试验中,M-CSF以及Ca125和UGP可能作为补充的时间生物学标记物,可以实现这一目标。
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