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Consequences of widespread deregulation of the c-myc gene in transgenic mice: multiple neoplasms and normal development.

作者信息

Leder A, Pattengale P K, Kuo A, Stewart T A, Leder P

出版信息

Cell. 1986 May 23;45(4):485-95. doi: 10.1016/0092-8674(86)90280-1.

Abstract

We have constructed a transgenic mouse strain in which a mammary tumor virus LTR/c-myc fusion gene is anomalously expressed in a wide variety of tissues. The deregulated c-myc transgene, now glucocorticoid inducible, contributes to an increased incidence of a variety of tumors, including those of testicular, breast, lymphocytic (B cell and T cell), and mast cell origin. The deregulated gene does not, however, otherwise disturb cell proliferation, nor does it interfere with normal development in these animals. Moreover, since not all tissues that express the transgene develop neoplasms, these results begin to define the transforming spectrum of the c-myc oncogene. They also extend to several organ systems the notion that elements in addition to an activated c-myc gene are required to induce malignancy in the living organism.

摘要

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