Bryan J. Boyle
Ford Motor Company
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Publication
Featured researches published by Bryan J. Boyle.
Journal of Molecular Evolution | 2005
Y. Tom Tang; Tianhua Hu; Matthew C. Arterburn; Bryan J. Boyle; Jessica M. Bright; Peter C. R. Emtage; Walter D. Funk
An emerging series of papers has identified new receptor proteins that predict seven-transmembrane pass topologies. We have consolidated this family to 11 human genes and have named the family PAQR, after two of the initially described ligands (progestin and adipoQ receptors). This protein family has ancient evolutionary roots, with identified homologs found in eubacteria. To date, published data indicate that the prokaryotic members of this family appear to encode hemolysin-type proteins, while in eukaryotes, PAQR proteins encode functional receptors with a broad range of apparent ligand specificities. We provide the complete human and mouse complement of this family, suggest a conserved structure/topology with invariant intracellular amino acid residues, and have measured mRNA expression levels for these genes across a range of human tissues.
Immunogenetics | 2002
Julio J. Mulero; Bryan J. Boyle; Shannon Bradley; Jessica M. Bright; Sarah T. Nelken; Tam T. Ho; Nancy K. Mize; John Childs; Dennis G. Ballinger; John E. Ford; Fabio Rupp
Abstract. We have identified three novel, rarely expressed human genes that encode new members of the lipid transfer/lipopolysaccharide binding protein (LT/LBP) gene family based on sequence homology. BPI and other members of the LT/LBP family are structurally related proteins capable of binding phospholipids and lipopolysaccharides. Real-time PCR studies indicate that BPIL1 and BPIL3 are highly expressed in hypertrophic tonsils. In situ hybridization analysis of BPIL2 shows prominent expression in skin specimens from psoriasis patients. BPIL1 and BPIL3 map to Chromosome 20q11; thus, these novel genes form a cluster with BPI and two other members of the LT/LBP gene family on the long arm of human Chr 20. BPIL2 maps to Chr 22q13. The exon/intron organization of all three genes is highly conserved with that of BPI, suggesting evolution from a common ancestor.
Science | 2005
Kyung-Ah Kim; Makoto Kakitani; Jingsong Zhao; Takeshi Oshima; Tom Y. Tang; Minke Binnerts; Yi Liu; Bryan J. Boyle; Emily Park; Peter C. R. Emtage; Walter Funk; Kazuma Tomizuka
Biochemical and Biophysical Research Communications | 2004
Minke Binnerts; Xiaohui Wen; Kirsten Canté-Barrett; Jessica M. Bright; Huang-Tsu Chen; Vinod Asundi; Peter Sattari; Tom Y. Tang; Bryan J. Boyle; Walter D. Funk; Fabio Rupp
Genomics | 2005
Y. Tom Tang; Tianhua Hu; Matthew C. Arterburn; Bryan J. Boyle; Jessica M. Bright; Servando Palencia; Peter C. R. Emtage; Walter D. Funk
Archive | 2004
Ivan Labat; Y. Tang; Birgit Stache-Crain; Bryan J. Boyle
Archive | 2002
Malabika Ghosh; Y. Tang; Jian-Rui Wang; Zhiwei Wang; Qing Zhao; Chongjun Xu; Julio J. Mulero; Bryan J. Boyle
Archive | 2001
John E. Ford; Bryan J. Boyle; Y. Tom Tang; Chenghua Liu; Vinod Asundi; Rui-Hong Chen; Yunqing Ma; Feiyan Ren; Jian-Rui Wang; Tom Werhman; Chongjun Xu; Aidong J. Xue; Yonghong Yang; Jie Zhang; Qing A. Zhao; Ping Zhou; Radoje T. Drmanac
Archive | 2000
Bryan J. Boyle; George Yeung; Matthew C. Arterburn; Nancy K. Mize; Y. Tom Tang; Chenghua Liu; Radoje Drmanac
Archive | 2000
Dana A. Haley; Bryan J. Boyle; Alice S. Ho; Matthew C. Arterburn; Y. Tom Tang; Chenghua Liu; Radoje T. Drmanac; Nancy K. Mize