CIRCADIAN VARIATIONS OF EPITHELIAL-CELL PROLIFERATION IN HUMAN RECTAL CRYPTS

被引:61
作者
MARRA, G
ANTI, M
PERCESEPE, A
ARMELAO, F
FICARELLI, R
COCO, C
RINELLI, A
VECCHIO, FM
DARCANGELO, E
机构
[1] UNIV CATTOLICA SACRO CUORE, DEPT SURG, I-00168 ROME, ITALY
[2] UNIV CATTOLICA SACRO CUORE, DEPT PATHOL, I-00168 ROME, ITALY
[3] UNIV ROMA LA SAPIENZA, DEPT STAT PROBABIL & APPL STAT, I-00185 ROME, ITALY
关键词
D O I
10.1016/0016-5085(94)90757-9
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
Background/Aims: Evidence (almost exclusively from animal studies) suggests that proliferation within the colorectal mucosa undergoes circadian variations. The epithelial cells that line the human colorectal crypt occupy definite positions along the longitudinal axis according to their proliferative potential and degree of differentiation. Thus, circadian rhymicity was investigated in humans to locate the areas along the longitudinal crypt axis in which diurnal fluctuation might occur. Methods: Rectal mucosal biopsy specimens were obtained every 4 hours for a 24-hour span from each of 23 subjects (8 healthy volunteers and 15 with histories of sporadic adenomatous polyps). [H-3]thymidine histoautoradiography was used to determine ratios of S-phase to total cells (total labeling index) in the crypt. Glands were also divided into 5 equal compartments from base (compartment 1) to mouth (compartment 5), and labeling indices were calculated for each. Results: Important temporal variations were confined to compartment 2 (F = 5.15, P = 0.0003) and total labeling indices (F = 3.57, P = 0.005). Despite individual variations, proliferation was generally higher at night and lower during afternoon. Upper-crypt proliferative rates (compartments 4 and 5) remained decidedly stable (F = 0.5, P = NS). Normal subjects and patients with polyps displayed similar circadian behaviors. Conclusions: Circadian fluctuation in proliferation is confined to the area of the crypt normally associated with replication. Upper-crypt indices, including those that were higher than normal (a colon-cancer risk marker) are stable over 24 hours. These findings should be useful in planning chemoprevention trials and chemotherapeutic regimens.
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页码:982 / 987
页数:6
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