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Blood Level of B and CD4+ Lymphocytes Measured before Induction of an Experimental Tumor in Rats Predicts Tumor Progression and Survival
After an initial series of experiments indicated that early responses of B lymphocytes were important in controlling tumor metastases in two rat models of cancer (N. Quan et al. , Cancer Res., 59: 1080–1089, 1999), the present study assessed whether differences in the number of B lymphocytes that ar...
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Published in: | Cancer epidemiology, biomarkers & prevention biomarkers & prevention, 2000-06, Vol.9 (6), p.609-617 |
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Main Authors: | , , , |
Format: | Article |
Language: | English |
Subjects: | |
Online Access: | Get full text |
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Summary: | After an initial series of experiments indicated that early responses of
B lymphocytes were important in controlling tumor metastases in two rat
models of cancer (N. Quan et al. , Cancer Res.,
59: 1080–1089, 1999), the present study assessed
whether differences in the number of B lymphocytes that are normally
present in different individual rats before any tumor development could
predict tumor growth, metastases, and length of survival when tumor
challenge subsequently occurred. Repeated baseline measures of several
circulating lymphocyte subtypes ( i.e., natural killer,
B, CD4+, CD8+ lymphocytes) were made in individual inbred WAG
rats before any introduction of tumor cells, and stable baselines for
these subtypes were found. Animals were then injected with 2 ×
10 6 CC531 tumor cells (a syngeneic tumor) into the leg, and
the size of the resulting primary tumor measured. Primary tumors were
surgically removed 6–7 weeks after tumor-cell injection, and animals
then followed until death from metastases. In two experiments, the size
of the primary tumor as well as the length of time that animals
survived correlated with the pretumor percentage of certain lymphocyte
subtypes in peripheral blood before tumor-cell injection. Baseline
percentage of B lymphocytes was significantly negatively correlated
with the size of the primary tumor and was positively correlated with
the duration of survival. Baseline percentage of CD4+ lymphocytes
showed the opposite relationship, being positively correlated with
tumor size and negatively correlated with survival time, although these
correlations were lower than those for B lymphocytes. Percent B
lymphocytes in circulation also declined during tumor development. In
summary, a high percentage of endogenous peripheral blood B lymphocytes
predicted growth of smaller primary tumors and longer survival after
experimental tumor induction in a rat model, further suggesting that B
lymphocytes are involved in protection against development of certain
tumors. |
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ISSN: | 1055-9965 1538-7755 |