Your search keyword '"Taylor, Brian"' showing total 21 results

1. Retinoic Acid Regulates Donor Myeloid Immune Reconstitution after Allogeneic Hematopoietic Stem Cell Transplantation in Mice

Author

Li, Xinlei, primary, Zheng, Jianwei, additional, Zhou, Dian, additional, Limpert, Rachel, additional, Taylor, Brian, additional, Tian, Linlu, additional, Yu, Xue-Zhong, additional, Drobyski, William R., additional, and Chen, Xiao, additional

Published

2022

2. Analysis of clonotypic switch junctions reveals multiple myeloma originates from a single class switch event with ongoing mutation in the isotype-switched progeny

Author

Taylor, Brian J., Kriangkum, Jitra, Pittman, Julie A., Mant, Michael J., Reiman, Tony, Belch, Andrew R., and Pilarski, Linda M.

Published

2008

3. Impaired class switch recombination (CSR) in Waldenström macroglobulinemia (WM) despite apparently normal CSR machinery

Author

Kriangkum, Jitra, Taylor, Brian J., Strachan, Erin, Mant, Michael J., Reiman, Tony, Belch, Andrew R., and Pilarski, Linda M.

Published

2006

4. Overexpression of transcripts originating from the MMSET locus characterizes all t(4;14)(p16;q32)-positive multiple myeloma patients

Author

Keats, Jonathan J., Maxwell, Christopher A., Taylor, Brian J., Hendzel, Michael J., Chesi, Marta, Bergsagel, P.Leif, Larratt, Loree M., Mant, Michael J., Reiman, Tony, Belch, Andrew R., and Pilarski, Linda M.

Published

2005

5. Clonotypic IgM V/D/J sequence analysis in Waldenstrom macroglobulinemia suggests an unusual B-cell origin and an expansion of polyclonal B cells in peripheral blood

Author

Kriangkum, Jitra, Taylor, Brian J., Treon, Steven P., Mant, Michael J., Belch, Andrew R., and Pilarski, Linda M.

Published

2004

6. In multiple myeloma, t(4;14)(p16;q32) is an adverse prognostic factor irrespective of FGFR3 expression

Author

Keats, Jonathan J., Reiman, Tony, Maxwell, Christopher A., Taylor, Brian J., Larratt, Loree M., Mant, Michael J., Belch, Andrew R., and Pilarski, Linda M.

Published

2003

7. Persistent preswitch clonotypic myeloma cells correlate with decreased survival: evidence for isotype switching within the myeloma clone

Author

Reiman, Tony, Seeberger, Karen, Taylor, Brian J., Szczepek, Agnieszka J., Hanson, John, Mant, Michael J., Coupland, Robert W., Belch, Andrew R., and Pilarski, Linda M.

Published

2001

8. Targeting Intestinal Vitamin D Receptor Signaling to Mitigate Graft-Versus-Host Disease

Author

Taylor, Brian, primary, Du, Jie, additional, Dodge, Joseph, additional, Li, Yan Chun, additional, and Chen, Xiao, additional

Published

2018

9. Genetic Variations in Genomic HAS1 Direct Aberrant Pre-mRNA Splicing That Generates the Prognostically Significant HAS1Vb Intronic Splice Variant.

Author

Kriangkum, Jitra, primary, Ghosh, Anirban, primary, Taylor, Brian J., primary, and Pilarski, Linda M., primary

Published

2007

10. Genomic Instability in Multiple Myeloma: Inducible Transfectants Provide a Model To Define the Role of RHAMM and Centrosome/Mitotic Spindle Stability in Myelomagenesis.

Author

Taylor, Brian J., primary, Baigorri, Eva, primary, Hay, Mary, primary, Reiman, Tony, primary, Belch, Andrew R., primary, and Pilarski, Linda M., primary

Published

2006

11. Molecular Characterization of Clonotypic VDJ Sequences in Waldenstrom’s Macroglobulinemia Suggests Independent Transformation Events in the Development of Biclonal B Cells.

Author

Kriangkum, Jitra, primary, Taylor, Brian J., primary, Treon, Steven P., primary, Mant, Michael J., primary, Reiman, Tony, primary, Belch, Andrew R., primary, and Pilarski, Linda M., primary

Published

2006

12. Analysis of Clonotypic Switch Junctions Reveals Multiple Myeloma Originates from a Single Class Switch Event with Ongoing Mutation in the Isotype Switched Progeny.

Author

Taylor, Brian J., primary, Kriangkum, Jitra, primary, Keats, Jonathan J., primary, Pittman, Julie, primary, Reiman, Tony, primary, Belch, Andrew R., primary, and Pilarski, Linda M., primary

Published

2005

13. Microfluidic Devices for Molecular Monitoring of Clonotypic IgH VDJ Signatures and the T(4;14) Translocation in Multiple Myeloma.

Author

Pilarski, Linda M., primary, Kaigala, Govindkrishna V., primary, VanDjiken, Jaron, primary, Atrazhev, Alexey, primary, Taylor, Brian J., primary, Belch, Andrew R., primary, and Backhouse, Christopher J., primary

Published

2005

14. Clonotypic IgG B Cells in Waldenstrom Macroglobulinemia Cells Are Derived from Multiple Post-Transformed B Cells That Have Undergone Isotype Switch Recombination.

Author

Kriangkum, Jitra, primary, Taylor, Brian J., primary, Strachan, Erin, primary, Reiman, Tony, primary, Belch, Andrew R., primary, Mant, Michael J., primary, and Pilarski, Linda M., primary

Published

2005

15. Analysis of Validated Clonotypic Igh VDJ Sequences from a Large Cohort of MM Patients.

Author

Taylor, Brian J., primary, Keats, Jonathan J., primary, Strachan, Erin R., primary, Reiman, Tony, primary, Belch, Andrew R., primary, and Pilarski, Linda M., primary

Published

2005

16. Clonal Analysis of IgM Cells in Multiple Myeloma Patients Suggests the Co-Existence of Normal and Malignant Arms of the Myeloma Clone.

Author

Taylor, Brian J., primary, Ye, Ming, primary, Strachan, Erin R., primary, Tiffinger, Tara M., primary, Belch, Andrew R., primary, and Pilarski, Linda M., primary

Published

2004

17. VDJ-Switch Region Analysis in Multiple Myeloma Patients Reveals Homogeneity and Long-Term Stability of Switch Junctions, and Ongoing Mutation Upstream of Switch Mu.

Author

Taylor, Brian J., primary, Pittman, Julie A., primary, Belch, Andrew R., primary, and Pilarski, Linda M., primary

Published

2004

18. Altered Kinetics and Localization of MMSET Variants Suggests That RE-IIBP Overexpression Is a Unifying Event in t(4;14)(p16;q32) Multiple Myeloma.

Author

Keats, Jonathan J., primary, Maxwell, Christopher A., additional, Reiman, Tony, additional, Taylor, Brian J., additional, Mant, Michael J., additional, Belch, Andrew J., additional, and Pilarski, Linda M., additional

Published

2004

19. Mutator Genes UDG and AID Appear To Be Normal in Class-Switch Deficient and Clonally Homogeneous Waldenstrom’s Macroglobulinemias Having Either Germline or Hypermutated Clonotypic IgH VDJ.

Author

Kriangkum, Jitra, primary, Taylor, Brian J., primary, Strachan, Erin R., primary, Treon, Steven P., primary, Mant, Michael J., primary, Reiman, Tony, primary, Belch, Andrew R., primary, and Pilarski, Linda M., primary

Published

2004

20. Overexpression of transcripts originating from the MMSETlocus characterizes all t(4;14)(p16;q32)-positive multiple myeloma patients

Author

Keats, Jonathan J., Maxwell, Christopher A., Taylor, Brian J., Hendzel, Michael J., Chesi, Marta, Bergsagel, P.Leif, Larratt, Loree M., Mant, Michael J., Reiman, Tony, Belch, Andrew R., and Pilarski, Linda M.

Abstract

Multiple myeloma (MM) is a B-lineage malignancy characterized by diverse genetic subtypes and clinical outcomes. The recurrent immunoglobulin heavy chain (IgH) switch translocation, t(4;14)(p16;q32), is associated with poor outcome, though the mechanism is unclear. Quantitative reverse-transcription–polymerase chain reaction (RT-PCR) for proposed target genes on a panel of myeloma cell lines and purified plasma cells showed that only transcripts originating from the WHSC1/MMSET/NSD2gene are uniformly dysregulated in all t(4;14)POSpatients. The different transcripts detected, multiple myeloma SET domain containing protein (MMSET I), MMSET II, Exon 4a/MMSET III, and response element II binding protein (RE-IIBP), are produced by alternative splicing and alternative transcription initiation events. Translation of the various transcripts, including those from major breakpoint region 4-2 (MB4-2) and MB4-3 breakpoint variants, was confirmed by transient transfection and immunoblotting. Green fluorescent protein (GFP)–tagged MMSET I and II, corresponding to proteins expressed in MB4-1 patients, localized to the nucleus but not nucleoli, whereas the MB4-2 and MB4-3 proteins concentrate in nucleoli. Cloning and localization of the Exon 4a/MMSET III splice variant, which contains the protein segment lost in the MB4-2 variant, identified a novel protein domain that prevents nucleolar localization. Kinetic studies using photobleaching suggest that the breakpoint variants are functionally distinct from wild-type proteins. In contrast, RE-IIBP is universally dysregulated and also potentially functional in all t(4;14)POSpatients irrespective of fibroblast growth factor receptor 3 (FGFR3) expression or breakpoint type.

Published

2005

21. Receptor Specificity of Clinical Plasmodium falciparum Isolates: Nonadherence to Cell-Bound E-Selectin and Vascular Cell Adhesion Molecule-1

Author

Udomsangpetch, Rachanee, Taylor, Brian J., Looareesuwan, Sornchai, White, Nicholas J., Elliott, John F., and Ho, May

Published

1996