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41 results on '"Yancopoulos, Sophia"'

1. Correction to: Intraclonal Complexity in Chronic Lymphocytic Leukemia: Fractions Enriched in Recently Born/Divided and Older/Quiescent Cells

Author

Calissano, Carlo, Damle, Rajendra N., Marsilio, Sonia, Yan, Xiao-Jie, Yancopoulos, Sophia, Hayes, Gregory, Emson, Claire, Murphy, Elizabeth J., Hellerstein, Marc K., Sison, Cristina, Kaufman, Matthew S., Kolitz, Jonathan E., Allen, Steven L., Rai, Kanti R., Ivanovic, Ivana, Dozmorov, Igor M., Roa, Sergio, Scharff, Matthew D., Li, Wentian, and Chiorazzi, Nicholas

Published
2022
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2. Myeloid-derived suppressor cell subtypes differentially influence T-cell function, T-helper subset differentiation, and clinical course in CLL

Author

Ferrer, Gerardo, Jung, Byeongho, Chiu, Pui Yan, Aslam, Rukhsana, Palacios, Florencia, Mazzarello, Andrea Nicola, Vergani, Stefano, Bagnara, Davide, Chen, Shih-Shih, Yancopoulos, Sophia, Xochelli, Aliki, Yan, Xiao-Jie, Burger, Jan A., Barrientos, Jacqueline C., Kolitz, Jonathan E., Allen, Steven L., Stamatopoulos, Kostas, Rai, Kanti R., Sherry, Barbara, and Chiorazzi, Nicholas

Published
2021
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3. The rise and fall of breakpoint reuse depending on genome resolution

Author

Attie, Oliver, Darling, Aaron E, and Yancopoulos, Sophia

Abstract

Abstract Background During evolution, large-scale genome rearrangements of chromosomes shuffle the order of homologous genome sequences ("synteny blocks") across species. Some years ago, a controversy erupted in genome rearrangement studies over whether rearrangements recur, causing breakpoints to be reused. Methods We investigate this controversial issue using the synteny block's for human-mouse-rat reported by Bourque et al. and a series of synteny blocks we generated using Mauve at resolutions ranging from coarse to very fine-scale. We conducted analyses to test how resolution affects the traditional measure of the breakpoint reuse rate. Results We found that the inversion-based breakpoint reuse rate is low at fine-scale synteny block resolution and that it rises and eventually falls as synteny block resolution decreases. By analyzing the cycle structure of the breakpoint graph of human-mouse-rat synteny blocks for human-mouse and comparing with theoretically derived distributions for random genome rearrangements, we showed that the implied genome rearrangements at each level of resolution become more “random” as synteny block resolution diminishes. At highest synteny block resolutions the Hannenhalli-Pevzner inversion distance deviates from the Double Cut and Join distance, possibly due to small-scale transpositions or simply due to inclusion of erroneous synteny blocks. At synteny block resolutions as coarse as the Bourque et al. blocks, we show the breakpoint graph cycle structure has already converged to the pattern expected for a random distribution of synteny blocks. Conclusions The inferred breakpoint reuse rate depends on synteny block resolution in human-mouse genome comparisons. At fine-scale resolution, the cycle structure for the transformation appears less random compared to that for coarse resolution. Small synteny blocks may contain critical information for accurate reconstruction of genome rearrangement history and parameters.

Published
2011

4. CLL stereotyped B-cell receptor immunoglobulin sequences are recurrent in the B-cell repertoire of healthy individuals: Apparent lack of central and early peripheral tolerance censoring

Author

Vergani, Stefano, primary, Bagnara, Davide, additional, Agathangelidis, Andreas, additional, Ng, Anita Kar Yun, additional, Ferrer, Gerardo, additional, Mazzarello, Andrea N., additional, Palacios, Florencia, additional, Yancopoulos, Sophia, additional, Yan, Xiao-Jie, additional, Barrientos, Jaqueline C., additional, Rai, Kanti R., additional, Stamatopoulos, Kostas, additional, and Chiorazzi, Nicholas, additional

Published
2023
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7. What Do Students Perceive during a Lesson on Center-of-Mass?

Author

Liby, Bruce W., Friedenberg, Jay, and Yancopoulos, Sophia

Abstract

This paper presents an assessment of how students perceive a typical classroom representation of center-of-mass. Participants were shown figures consisting of two filled black circles; they were told that these figures represented spheres or balls. They were then asked to indicate with a mark the point where the spheres would balance, i. e., they were asked to find the center-of-mass. There were two participant groups. The first group (labeled "Control") received only brief, written instructions on the exercise. The second group (labeled "COM") was shown a 15-minute video which discussed, qualitatively, the topic of center of mass and the same written instructions. They also received the same written instructions as the Control group. The results indicate how students perceive the problem. In all groups students do not estimate the center-of-mass as if they were considering spheres. We find that while the performance for both groups was poor, there is a difference between the two. This suggests some insight on teaching the topic. (Contains 3 figures.)

Published
2009

9. A seven-gene expression panel distinguishing clonal expansions of pre-leukemic and chronic lymphocytic leukemia B cells from normal B lymphocytes

Author

McCarthy, Brian A., Yancopoulos, Sophia, Tipping, Mike, Yan, Xiao-jie, Wang, Xue Ping, Bennett, Fiona, Li, Wentian, Lesser, Martin, Paul, Santanu, Boyle, Erin, Moreno, Carolina, Catera, Rosa, Messmer, Bradley T., Cutrona, Giovanna, Ferrarini, Manlio, Kolitz, Jonathan E., Allen, Steven L., Rai, Kanti R., Rawstron, Andrew C., and Chiorazzi, Nicholas

Published
2015
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15. Intraclonal Complexity in Chronic Lymphocytic Leukemia: Fractions Enriched in Recently Born/Divided and Older/Quiescent Cells

Author

Calissano, Carlo, Damle, Rajendra N., Marsilio, Sonia, Yan, Xiao-Jie, Yancopoulos, Sophia, Hayes, Gregory, Emson, Claire, Murphy, Elizabeth J., Hellerstein, Marc K., Sison, Cristina, Kaufman, Matthew S., Kolitz, Jonathan E., Allen, Steven L., Rai, Kanti R., Ivanovic, Ivana, Dozmorov, Igor M., Roa, Sergio, Scharff, Matthew D., Li, Wentian, and Chiorazzi, Nicholas

Published
2011
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18. The rise and fall of breakpoint reuse depending on genome resolution

Author

Darling Aaron E, Attie Oliver, and Yancopoulos Sophia

Subjects
Computer applications to medicine. Medical informatics, R858-859.7, Biology (General), QH301-705.5
Abstract

Abstract Background During evolution, large-scale genome rearrangements of chromosomes shuffle the order of homologous genome sequences ("synteny blocks") across species. Some years ago, a controversy erupted in genome rearrangement studies over whether rearrangements recur, causing breakpoints to be reused. Methods We investigate this controversial issue using the synteny block's for human-mouse-rat reported by Bourque et al. and a series of synteny blocks we generated using Mauve at resolutions ranging from coarse to very fine-scale. We conducted analyses to test how resolution affects the traditional measure of the breakpoint reuse rate. Results We found that the inversion-based breakpoint reuse rate is low at fine-scale synteny block resolution and that it rises and eventually falls as synteny block resolution decreases. By analyzing the cycle structure of the breakpoint graph of human-mouse-rat synteny blocks for human-mouse and comparing with theoretically derived distributions for random genome rearrangements, we showed that the implied genome rearrangements at each level of resolution become more “random” as synteny block resolution diminishes. At highest synteny block resolutions the Hannenhalli-Pevzner inversion distance deviates from the Double Cut and Join distance, possibly due to small-scale transpositions or simply due to inclusion of erroneous synteny blocks. At synteny block resolutions as coarse as the Bourque et al. blocks, we show the breakpoint graph cycle structure has already converged to the pattern expected for a random distribution of synteny blocks. Conclusions The inferred breakpoint reuse rate depends on synteny block resolution in human-mouse genome comparisons. At fine-scale resolution, the cycle structure for the transformation appears less random compared to that for coarse resolution. Small synteny blocks may contain critical information for accurate reconstruction of genome rearrangement history and parameters.

Published
2011
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24. Comparative Density Analyses of B Cell Receptor-Complex Components (Membrane IgM, Membrane IgD, and Stimulatory/Inhibitory Co-Receptors) on Intraclonal Subpopulations of CLL B Cells, before and during Ibrutinib Therapy

Author

Mazzarello, Andrea Nicola, primary, Vergani, Stefano, additional, Ferrer, Gerardo, additional, Liu, Yun, additional, Chen, Shih-Shih, additional, Yancopoulos, Sophia, additional, Yan, Xiao-Jie, additional, Barrientos, Jacqueline C., additional, Rai, Kanti R., additional, and Chiorazzi, Nicholas, additional

Published
2016
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25. B Cells of the Proliferative Fraction of CLL Clones Exhibit Activated B-Cell and Myeloid-Cell Signatures Suggesting Enhanced Antigen-Presentation, Integrin Responsiveness, and IL-4 Receptiveness: Additional Targets for CLL Therapy

Author

Yan, Xiao-Jie, primary, Palacios, Florencia, additional, Li, Wentian, additional, Yancopoulos, Sophia, additional, Calissano, Carlo, additional, Barrientos, Jacqueline C., additional, Allen, Steven L., additional, Kolitz, Jonathan E., additional, Rai, Kanti, additional, and Chiorazzi, Nicholas, additional

Published
2016
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26. In CLL, Myeloid-Derived Suppressor Cells and Their Monocytic and Granulocytic Varieties Differ in T-Cell Subset Association and Polarization Induction

Author

Ferrer, Gerardo, primary, Franca, Brendan, additional, Chiu, Pui Yan, additional, Vergani, Stefano, additional, Mazzarello, Andrea Nicola, additional, Palacios, Florencia, additional, Bagnara, Davide, additional, Chen, Shih-Shih, additional, Yancopoulos, Sophia, additional, Liu, Yun, additional, Xochelli, Aliki, additional, Yan, Xiao-Jie, additional, Barrientos, Jacqueline C., additional, Kolitz, Jonathan E., additional, Allen, Steven L., additional, Stamatopoulos, Kostas, additional, Rai, Kanti R., additional, Sherry, Barbara, additional, and Chiorazzi, Nicholas, additional

Published
2016
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28. Myeloid-Derived Suppressor Cell Subtypes Are Responsible for the Th2 Phenotype of T Cells in CLL

Author

Ferrer, Gerardo, Franca, Brendan, Chiu, Pui Yan, Vergani, Stefano, Mazzarello, Andrea Nicola, Palacios, Florenca, Chen, Shihshih, Bagnara, Davide, Yancopoulos, Sophia, Liu, Yun, Xochelli, Aliki, Yan, Xiao J., Kolitz, Jonathan E., Allen, Steven L., Barrientos, Jacqueline C., Stamatopoulos, Kostas, Rai, Kanti, Sherry, Barbara, and Chiorazzi, Nicholas

Published
2017
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31. A Systematic Search Into The Role Of IGHV Gene Replacement In Shaping The Immunoglobulin Repertoire Of Chronic Lymphocytic Leukemia

Author

Yancopoulos, Sophia, primary, Yan, Xiao-Jie, additional, Agathangelidis, Andreas, additional, Li, Wentian, additional, Belessi, Chrysoula, additional, Ghia, Paolo, additional, Rosenquist, Richard, additional, Davi, Frederic, additional, Oscier, David Graham, additional, Pospisilova, Sarka, additional, Panagiotidis, Panagiotis, additional, Huang, Lin, additional, Zhang, Zhixin, additional, Allen, Steven L., additional, Barrientos, Jaqueline C., additional, Kolitz, Jonathan E., additional, Rai, Kanti R., additional, Stamatopoulos, Kostas, additional, and Chiorazzi, Nicholas, additional

Published
2013
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32. Gene Expression Profiles Document That Recently- and Previously-Divided CLL Fractions Represent a Continuum but Suggest Differing Modes of Activation for These Fractions in U-CLL and M-CLL

Author

Yan, Xiao J., primary, Li, Wentian, additional, Yancopoulos, Sophia, additional, Dozmorov, Igor, additional, Calissano, Carlo, additional, Marsilio, Sonia, additional, Damle, Rajendra N, additional, Allen, Steven L., additional, Kolitz, Jonathan E., additional, Barrientos, Jacqueline C., additional, Rai, Kanti R., additional, and Chiorazzi, Nicholas, additional

Published
2012
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33. Combining Expression of Hypervariably Expressed Genes with IGHV Mutation Status Is a More Robust Prognostic Indicator Than Mutation Status Alone in Chronic Lymphocytic Leukemia

Author

Yan, Xiao J., primary, Dozmorov, Igor, additional, Ivana, Ivanovic, additional, Yancopoulos, Sophia, additional, Kalenscher, Daniel, additional, Boyle, Erin, additional, Damle, Aarti, additional, Damle, Rajendra N, additional, Chu, Charles C., additional, Khalili, Houman, additional, Lee, Annette, additional, Li, Wentian, additional, Gregersen, Peter, additional, Sison, Cristina, additional, Lesser, Martin L, additional, Kaufman, Matthew, additional, Allen, Steven L., additional, Kolitz, Jonathan E., additional, Rai, Kanti R., additional, and Chiorazzi, Nicholas, additional

Published
2011
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34. Gene Set Enrichment Analysis of Ki-67high CLL Clones Suggests Complex Interactions of B-Cell Receptor Signaling and Normal Cell Interactions in the Disease

Author

Yan, Xiao J., primary, Kalenscher, Daniel, additional, Boyle, Erin, additional, Yancopoulos, Sophia, additional, Damle, Rajendra N, additional, Damle, Aarti, additional, Khalili, Houman, additional, Lee, Annette, additional, Li, Wentian, additional, Dozmorov, Igor, additional, Kaufman, Matthew, additional, Gregersen, Peter, additional, Allen, Steven L., additional, Kolitz, Jonathan E., additional, Rai, Kanti R., additional, and Chiorazzi, Nicholas, additional

Published
2011
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35. 1.16 Gene Set Enrichment Analysis of CLL Subgroups Defined by Ki-67 Expression

Author

Yan, Xiao-Jie, primary, Kalenscher, Daniel, additional, Boyle, Erin, additional, Damle, Arrti, additional, Yancopoulos, Sophia, additional, Damle, Rajendra N., additional, Khalili, Houman, additional, Lee, Annette, additional, Li, Wentian, additional, Dozmorov, Igor, additional, Kaufman, Matthew, additional, Gregersen, Peter, additional, Allen, Steven L., additional, Rai, Kanti R., additional, and Chiorazzi, Nicholas, additional

Published
2011
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38. Genome Analysis of CLL by Representational Oligonucleotide Microarray Analysis (ROMA).

Author

Grubor, Vladimir D., primary, Troge, Jennifer E., additional, Meth, Jennifer L., additional, Lakshmi, B., additional, Yamron, Boris, additional, Hufnagel, Lisa A., additional, Lee, Yoon-Ha, additional, Kendall, Jude T., additional, Pai, Deepa, additional, Lee, Annette, additional, Gregersen, Peter, additional, Yancopoulos, Sophia, additional, Allen, Steven, additional, Rai, Kanti R., additional, Chiorazzi, Nicholas, additional, Wigler, Michael H., additional, and Esposito, Diane, additional

Published
2006
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40. B cell receptors in TCL1 transgenic mice resemble those of aggresive, treatment-resistant human chronic lymphoytic leukemia.

Author

Xiao-Jie Yan, Albesiano, Emilia, Zanesi, Nicola, Yancopoulos, Sophia, Sawyer, Alan, Romano, Egidio, Petlickovski, Aleksandar, Efremov, Dimitar G., Croce, Carlo M., and Chiorazzi, Nicholas

Subjects
B cells, CHRONIC lymphocytic leukemia, LYMPHOCYTE receptors, CHRONIC diseases, LYMPHOCYTIC leukemia, GENE expression
Abstract

B cell chronic lymphocytic leukemia (B-CLL) is a clonal overgrowth of CD5+ B lymphocytes. In this disease, the B cell antigen receptor (BCR) is intimately linked to disease severity, because patients with BCRs, comprised of unmutated VH genes, follow a much more aggressive course. This and related observations suggest that B-CLL derives from a B cell subset comprised of restricted BCR structural diversity and that antigen-selection and drive are major factors promoting the disease. Nevertheless, the initiating event(s) that lead to the development of B-CLL are still unclear, in part because of the lack of an animal model that spontaneously evolves the molecular abnormalities that occur in the human disease. Because overexpression of the TCL1 gene in murine B cells leads to a CD5+ B cell lymphoproliferative disorder with many of the features of human B-CLL, we studied leukemias emerging in these mice to examine the extent to which their BCRs resemble those in B-CLL. Our data indicate that the immunoglobulin heavy and light chain rearrangements in TCL1 mice display minimal levels of somatic mutations and exhibit several molecular features found in the human disease. Like human B-CLL, TCL1 leukemic rearrangements from different mice can be very similar structurally and closely resemble autoantibodies and antibodies reactive with microbial antigens. Antigen-binding analyses confirm that selected TCL1 clones react with glycerophospholipid, lipoprotein, and polysaccharides that can be autoantigens and be expressed by microbes. This (auto)antigen-driven mouse model reliably captures the BCR characteristics of aggressive, treatment-resistant human B-CLL. [ABSTRACT FROM AUTHOR]

Published
2006
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41. Gene Set Enrichment Analysis of Ki-67highCLL Clones Suggests Complex Interactions of B-Cell Receptor Signaling and Normal Cell Interactions in the Disease

Author

Yan, Xiao J., Kalenscher, Daniel, Boyle, Erin, Yancopoulos, Sophia, Damle, Rajendra N, Damle, Aarti, Khalili, Houman, Lee, Annette, Li, Wentian, Dozmorov, Igor, Kaufman, Matthew, Gregersen, Peter, Allen, Steven L., Kolitz, Jonathan E., Rai, Kanti R., and Chiorazzi, Nicholas

Abstract

Abstract 2833

Published
2011
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