Gene/Protein Disease Symptom Drug Enzyme Compound
Pivot Concepts:   Target Concepts:
Query: UMLS:C0038002 (splenomegaly)
 9,873 document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)

The hematopoietic disregulation in adult mice induced by the malignant histiocytosis sarcoma virus (MHSV) and the Harvey murine sarcoma virus (Ha-MuSV), which both possess c-Ha-ras-related oncogenic sequences, was investigated. Spleen focus formation induced by MHSV and Ha-MuSV was not restricted by the Fv-2 resistance locus in congenic DDD and C57BL/6 mice, unlike leukemogenesis induced by Friend virus, Rauscher virus, and the myeloproliferative sarcoma virus (MPSV). C57BL/6 mice were much more resistant to MHSV and Ha-MuSV-induced spleen focus formation than DDD mice regardless of their Fv-2 state. Infection of DDD mice with MHSV caused a systemic histiocytic neoplasia, best described as murine malignant histiocytosis. Transformed histiocytic cells proliferated excessively in the bone marrow, spleen, and lymph nodes and, in the final stages of the disease, in all major parenchymal organs. The Ha-MuSV caused a strikingly different benign histiocytic tumor in DDD mice and, unlike MHSV, did not induce a rapid, progressive splenomegaly in C57BL/6 mice. Infection of DDD mice with MHSV induced a rapid and synchronized depletion of early and late erythroid precursor cell pools. In MHSV-infected C57BL/6 mice comparable changes were observed with dissimilar kinetics. Macrophage colony-forming cells of MHSV-infected mice were increased in number and proliferated independently of stimulating growth factors. The disease induced by MHSV in mice can thus serve as a model for malignant histiocytosis in humans.
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PMID:Murine retrovirus-induced malignant histiocytosis, an experimental model for the disease in humans. 282 12

Cellular ras oncogenes transduced by retroviruses carry mutations in amino acids 12, 59 and 122. Similar mutations have been observed in ras oncogenes activated during induction of neoplasia in both humans and experimental animals. The unmutated normal rat or human c-Ha-ras-1 genes have the ability to transform NIH 3T3 cells in culture when activated by a RNA synthesis promoter. These findings raise the question of whether the mutations are necessary for the ras oncogenes to induce the neoplastic phenotype in vivo. To address this question, we inserted the normal human c-Ha-ras-1 or its mutated counterpart EJ/T24 bladder carcinoma oncogene independently into a retrovirus vector derived from the M1 strain of Moloney murine sarcoma virus (MoMuSV). Both recombinant clones induced foci of transformed cells in an NIH 3T3 cell transfection assay. Infectious virus particles were rescued from cloned transformants carrying a single copy of the integrated provirus using the nonpathogenic amphotrophic wild mouse leukemia virus (WMLV) as helper. The pseudotypes rescued from the EJ/T24-containing transformants had higher titers than the normal c-Ha-ras-1 pseudotypes as determined by a focus assay and gave rise to larger and earlier detected foci upon infection of NIH 3T3 cells. The two pseudotypes were tested for in vivo pathogenicity by inoculation into newborn NFS mice and were compared to the pseudotype WMLV/Harvey murine sarcoma virus (HaMuSV) (positive control) and WMLV (negative control). While the WMLV/EJ/T24 and the WMLV/HaMuSV pseudotypes induced erythroleukemias and sarcomas with a latency period of 6-9 weeks, the WMLV/c-Ha-ras-1 pseudotype induced only mild splenomegaly. As expected the WMLV negative control induced no pathology. Tumor-bearing animals that were not euthanized at 6-9 weeks died within 2-3 months following virus inoculation.
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PMID:Pathogenicity of retroviruses containing either the normal human c-Ha-ras1 gene or its mutated form derived from the bladder carcinoma EJ/T24 cell line. 384 94