International Journal of Cell Cloning, Vol 10, 196-204, Copyright © 1992 by AlphaMed Press
The molecular control of hematopoiesis: from clonal development in culture to therapy in the clinic
L Sachs
Department of Molecular Genetics and Virology, Weizmann Institute of Science, Rehovot, Israel.
The establishment of a cell culture system for the clonal development of
hematopoietic cells has made it possible to discover the proteins that
regulate cell viability, growth and differentiation of different
hematopoietic cell lineages and the molecular basis of normal and abnormal
cell development in blood-forming tissues. These regulators include
cytokines now called colony stimulating factors and interleukins. Different
cytokines can induce cell viability, multiplication and differentiation,
and hematopoiesis is controlled by a network of interactions between these
cytokines. This network includes positive regulators such as colony
stimulating factors and interleukins and negative regulators such as
transforming growth factor beta and tumor necrosis factor. Gene cloning has
shown that there is a family of different genes for these cytokines. The
functioning of the network requires an appropriate balance between positive
and negative regulators and the selective regulation of programmed cell
death (apoptosis). There are different ways of inducing or inhibiting
programmed cell death, and differences in the regulation of this program
can result in tumor promotion or tumor suppression. The cytokine network
which has arisen during evolution allows considerable flexibility,
depending on which part of the network is activated and the ready
amplification of response to a particular stimulus. A network may also be
necessary to stabilize the whole system. Cytokines that regulate
hematopoiesis can induce the expression of genes for transcription factors
can thus ensure the autoregulation and transregulation of cytokine genes
that occur in the network.(ABSTRACT TRUNCATED AT 250 WORDS)
