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Start Over Author "Williams, B. P." Journal oncogene
8 results on '"Williams, B. P."'

6. Mice deleted for cell division cycle 73 gene develop parathyroid and uterine tumours: model for the hyperparathyroidism-jaw tumour syndrome

Author

Walls, G V, Stevenson, M, Lines, K E, Newey, P J, Reed, A A C, Bowl, M R, Jeyabalan, J, Harding, B, Bradley, K J, Manek, S, Chen, J, Wang, P, Williams, B O, Teh, B T, and Thakker, R V

Abstract

The hyperparathyroidism-jaw tumour (HPT-JT) syndrome is an autosomal dominant disorder characterized by occurrence of parathyroid tumours, often atypical adenomas and carcinomas, ossifying jaw fibromas, renal tumours and uterine benign and malignant neoplasms. HPT-JT is caused by mutations of the cell division cycle 73 (CDC73) gene, located on chromosome 1q31.2 and encodes a 531 amino acid protein, parafibromin. To facilitate in vivo studies of Cdc73 in tumourigenesis we generated conventional (Cdc73+/−) and conditional parathyroid-specific (Cdc73+/L/PTH-Cre and Cdc73L/L/PTH-Cre) mouse models. Mice were aged to 18-21 months and studied for survival, tumour development and proliferation, and serum biochemistry, and compared to age-matched wild-type (Cdc73+/+and Cdc73+/+/PTH-Cre) littermates. Survival of Cdc73+/−mice, when compared to Cdc73+/+mice was reduced (Cdc73+/−=80%; Cdc73+/+=90% at 18 months of age, P<0.05). Cdc73+/−, Cdc73+/L/PTH-Cre and Cdc73L/L/PTH-Cre mice developed parathyroid tumours, which had nuclear pleomorphism, fibrous septation and increased galectin-3 expression, consistent with atypical parathyroid adenomas, from 9 months of age. Parathyroid tumours in Cdc73+/−, Cdc73+/L/PTH-Cre and Cdc73L/L/PTH-Cre mice had significantly increased proliferation, with rates >fourfold higher than that in parathyroid glands of wild-type littermates (P<0.0001). Cdc73+/−, Cdc73+/L/PTH-Cre and Cdc73L/L/PTH-Cre mice had higher mean serum calcium concentrations than wild-type littermates, and Cdc73+/−mice also had increased mean serum parathyroid hormone (PTH) concentrations. Parathyroid tumour development, and elevations in serum calcium and PTH, were similar in males and females. Cdc73+/−mice did not develop bone or renal tumours but female Cdc73+/−mice, at 18 months of age, had uterine neoplasms comprising squamous metaplasia, adenofibroma and adenomyoma. Uterine neoplasms, myometria and jaw bones of Cdc73+/−mice had increased proliferation rates that were 2-fold higher than in Cdc73+/+mice (P<0.05). Thus, our studies, which have established mouse models for parathyroid tumours and uterine neoplasms that develop in the HPT-JT syndrome, provide in vivo models for future studies of these tumours.

Published
2017
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7. Myeloid-specific TGF-ß signaling in bone promotes basic-FGF and breast cancer bone metastasis

Author

Meng, X, Vander Ark, A, Lee, P, Hostetter, G, Bhowmick, N A, Matrisian, L M, Williams, B O, Miranti, C K, and Li, X

Abstract

Breast cancer (BCa) bone metastases cause osteolytic bone lesions, which result from the interactions of metastatic BCa cells with osteoclasts and osteoblasts. Osteoclasts differentiate from myeloid lineage cells. To understand the cell-specific role of transforming growth factor beta (TGF-ß) in the myeloid lineage, in BCa bone metastases, MDA-MB-231 BCa cells were intra-tibially or intra-cardially injected into LysMCre/Tgfbr2floxE2/floxE2knockout (LysMCre/Tgfbr2KO) or Tgfbr2floxE2/floxE2mice. Metastatic bone lesion development was compared by analysis of both lesion number and area. We found that LysMCre/Tgfbr2knockout significantly decreased MDA-MB-231 bone lesion development in both the cardiac and tibial injection models. LysMCre/Tgfbr2knockout inhibited the tumor cell proliferation, angiogenesis and osteoclastogenesis of the metastatic bones. Cytokine array analysis showed that basic fibroblast growth factor (bFGF) was downregulated in MDA-MB-231-injected tibiae from the LysMCre/Tgfbr2KO group, and intravenous injection of the recombinant bFGF to LysMCre/Tgfbr2KO mice rescued the inhibited metastatic bone lesion development. The mechanism by which bFGF rescued the bone lesion development was by promotion of tumor cell proliferation through the downstream mitogen-activated protein kinase (MAPK)-extracellular signal–regulated kinase (ERK)-cFos pathway after binding to the FGF receptor 1 (FGFR1). Consistent with animal studies, we found that in human BCa bone metastatic tissues, TGF-ß type II receptor (TßRII) and p-Smad2 were expressed in osteoclasts and tumor cells, and were correlated with the expression of FGFR1. Our studies suggest that myeloid-specific TGF-ß signaling-mediated bFGF in the bone promotes BCa bone metastasis.

Published
2016
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8. A human sequence homologous to v-sea maps to chromosome 11, band q13.

Author

Williams BP, Shipley JP, Spurr NK, Smith DR, Hayman MJ, and Goodfellow PN

Subjects
Chromosome Mapping, Humans, Hybrid Cells analysis, Lymphocytes analysis, Nucleic Acid Hybridization, Restriction Mapping, Sequence Homology, Nucleic Acid, Chromosomes, Human, Pair 11 ultrastructure, Oncogene Proteins, Viral genetics
Abstract

Human sequences homologous to the v-sea oncogene have been localised in the human genome to the region 11q13. This region of the genome has been implicated in chronic lymphocytic leukaemia and also encodes the INT-2 human oncogene.

Published
1988

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