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1. Megakaryocytes compensate for Kit insufficiency in murine arthritis

Author

Cunin, Pierre, Penke, Loka R., Thon, Jonathan N., Monach, Paul A., Jones, Tatiana, Chang, Margaret H., Chen, Mary M., Melki, Imene, Lacroix, Steve, Iwakura, Yoichiro, Ware, Jerry, Gurish, Michael F., Italiano, Joseph E., Boilard, Eric, and Nigrovic, Peter A.

Subjects
Bone marrow cells -- Research, Mast cells -- Research, Arthritis -- Research, Health care industry
Abstract

The growth factor receptor Kit is involved in hematopoietic and nonhematopoietic development. Mice bearing Kit defects lack mast cells; however, strains bearing different Kit alleles exhibit diverse phenotypes. Herein, we investigated factors underlying differential sensitivity to IgG-mediated arthritis in 2 mast cell-deficient murine lines: [Kit.sup.Wsh/Wsh], which develops robust arthritis, and [Kit.sup.W/Wv], which does not. Reciprocal bone marrow transplantation between [Kit.sup.W/Wv] and [Kit.sup.Wsh/Wsh] mice revealed that arthritis resistance reflects a hematopoietic defect in addition to mast cell deficiency. In [Kit.sup.W/Wv] mice, restoration of susceptibility to IgG-mediated arthritis was neutrophil independent but required IL-1 and the platelet/ megakaryocyte markers NF-E2 and glycoprotein VI. In [Kit.sup.W/Wv] mice, platelets were present in numbers similar to those in WT animals and functionally intact, and transfer of WT platelets did not restore arthritis susceptibility. These data implicated a platelet-independent role for the megakaryocyte, a Kit-dependent lineage that is selectively deficient in [Kit.sup.W/Wv] mice. Megakaryocytes secreted IL-1 directly and as a component of circulating microparticles, which activated synovial fibroblasts in an IL-1-dependent manner. Transfer of WT but not IL-1-deficient megakaryocytes restored arthritis susceptibility to [Kit.sup.W/Wv] mice. These findings identify functional redundancy among Kit-dependent hematopoietic lineages and establish an unanticipated capacity of megakaryocytes to mediate IL-1-driven systemic inflammatory disease., Introduction Mast cells (MCs) were first described as tissue-resident cells that stain brightly with aniline dyes (1). Their highly granular appearance reflects their capacity to release a wide range of [...]

Published
2017
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2. Lintuzumab-Ac225 with Combination with Intensive Chemotherapy Yields High Response Rate and MRD Negativity in R/R AML with Adverse Features

Author

Abedin, Sameem, primary, Guru Murthy, Guru Subramanian, additional, Szabo, Aniko, additional, Hamadani, Mehdi, additional, Michaelis, Laura C., additional, Carlson, Karen-Sue, additional, Runaas, Lyndsey, additional, Gauger, Katelyn, additional, Desai, Avinash G, additional, Chen, Mary M, additional, Harrington, Alexandra M., additional, and Atallah, Ehab L., additional

Published
2022
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4. Evaluating the Impact of a Community College's Strategic Enrollment Management (SEM) Model on High School Student Recruitment

Author

Chen, Mary M. Y.

Abstract

Community colleges are always looking to find ways to increase enrollment, either through recruitment of new students or retention of current students. This research is focused on the recruitment of new students--specifically high school students--using a Strategic Enrollment Management (SEM) model: nurturing high school students through the application process and deploying teams to local high schools to facilitate the admission process on site. The purpose of the study is to determine how the use of a SEM model at a mainstream comprehensive high school impacts overall Delaware Technical and Community College (DTCC) enrollment from a feeder school, High School A (HS A), and more specifically, enrollment in DTCC's engineering program, an under-enrolled program. Positive feedback was received from the HS A participants that the outreach message was well received. Connected Degree (a program to parlay the 2-year into a 4-year degree) and financial aid continued to be the two most important subjects for HS A participants for all years. However, despite the positive feedback, enrollment numbers from HS A declined. Based on the data collected, the SEM model treatment had no impact on overall enrollment numbers from HS A. Unlike overall enrollment numbers, engineering enrollment numbers fluctuated among all schools during the SEM model time frame, and based on these results, there seemed to be no positive impact on engineering enrollment after using the SEM model plus engineering component treatment. There was no negative impact either, so the result is unclear as to how the SEM model impacted engineering enrollment. Because of the quasi-experimental nature of the study outside variables were introduced that may have influenced the outcomes of the treatment. Factors like the economy perhaps had an impact that was unplanned. [The dissertation citations contained here are published with the permission of ProQuest LLC. Further reproduction is prohibited without permission. Copies of dissertations may be obtained by Telephone (800) 1-800-521-0600. Web page: http://www.proquest.com/en-US/products/dissertations/individuals.shtml.]

Published
2010

6. Endogenous regulation of cardiovascular function by apelin-APJ

Author

Charo, David N., Ho, Michael, Fajardo, Giovanni, Kawana, Masataka, Kundu, Ramendra K., Sheikh, Ahmad Y., Finsterbach, Thomas P., Leeper, Nicholas J., Ernst, Kavita V., Chen, Mary M., Ho, Yen Dong, Chun, Hyung J., Bernstein, Daniel, Ashley, Euan A., and Quertermous, Thomas

Subjects
Heart cells -- Genetic aspects, Heart cells -- Physiological aspects, Heart cells -- Research, Cardiovascular system -- Research, G proteins -- Physiological aspects, G proteins -- Research, Biological sciences
Abstract

Studies have shown significant cardiovascular effects of exogenous apelin administration, including the potent activation of cardiac contraction. However, the role of the endogenous apelin-APJ pathway is less clear. To study the loss of endogenous apelin-APJ signaling, we generated mice lacking either the ligand (apelin) or the receptor (APJ). Apelin-deficient mice were viable, fertile, and showed normal development. In contrast, APJ-deficient mice were not born in the expected Mendelian ratio, and many showed cardiovascular developmental defects. Under basal conditions, both apelin and APJ null mice that survived to adulthood manifested modest decrements in contractile function. However, with exercise stress both mutant lines demonstrated consistent and striking decreases in exercise capacity. To explain these findings, we explored the role of autocrine signaling in vitro using field stimulation of isolated left ventricular cardiomyocytes lacking either apelin or APJ. Both groups manifested less sarcomeric shortening and impaired velocity of contraction and relaxation with no difference in calcium transient. Taken together, these results demonstrate that endogenous apelin-APJ signaling plays a modest role in maintaining basal cardiac function in adult mice with a more substantive role during conditions of stress. In addition, an autocrine pathway seems to exist in myocardial cells, the ablation of which reduces cellular contraction without change in calcium transient. Finally, differences in the developmental phenotype between apelin and APJ null mice suggest the possibility of undiscovered APJ ligands or ligand-independent effects of APJ. pressure-volume hemodynamics; cardiomyocyte doi: 10.1152/ajpheart.00686.2009.

Published
2009

7. In vivo genetic profiling and cellular localization of apelin reveals a hypoxia-sensitive, endothelial-centered pathway activated in ischemic heart failure

Author

Sheikh, Ahmad Y., Chun, Hyung J., Glassford, Alexander J., Kundu, Ramendera K., Kutschka, Ingo, Ardigo, Diego, Hendry, Stephen L., Wagner, Roger A., Chen, Mary M., Ali, Ziad A., Yue, Patrick, Huynh, Diem T., Connolly, Andrew J., Pelletier, Marc P., Tsao, Philip S., Robbins, Robert C., and Quertermous, Thomas

Subjects
Myocardial ischemia -- Development and progression, Myocardial ischemia -- Physiological aspects, Myocardial ischemia -- Genetic aspects, Ligands (Biochemistry) -- Physiological aspects, Ligands (Biochemistry) -- Genetic aspects, Muscle contraction -- Properties, Gene expression -- Evaluation, Vascular endothelium -- Genetic aspects, Vascular endothelium -- Chemical properties, Biological sciences
Abstract

Signaling by the peptide ligand apelin and its cognate G protein-coupled receptor APJ has a potent inotropic effect on cardiac contractility and modulates systemic vascular resistance through nitric oxide-dependent signaling. In addition, there is evidence for counterregulation of the angiotensin and vasopressin pathways. Regulatory stimuli of the apelin-APJ pathway are of obvious importance but remain to be elucidated. To better understand the physiological response of apelin-APJ to disease states such as heart failure and to elucidate the mechanism by which such a response might occur, we have used the routine model of left anterior descending coronary artery ligation-induced ischemic cardiac failure. To identify the key cells responsible for modulation and production of apelin in vivo, we have created a novel apelin-lacZ reporter mouse. Data from these studies demonstrate that apelin and APJ are upregulated in the heart and skeletal muscle following myocardial injury and suggest that apelin expression remains restricted to the endothelium. In cardiac failure, endothelial apelin expression correlates with other hypoxia-responsive genes, and in healthy animals both apelin and APJ are markedly upregulated in various tissues following systemic hypoxic exposure. Experiments with cultured endothelial cells in vitro show apelin mRNA and protein levels to be increased by hypoxia, through a hypoxia-inducible factor-mediated pathway. These studies suggest that apelin-expressing endothelial cells respond to conditions associated with heart failure, possibly including local tissue hypoxia, and modulate apelin-APJ expression to regulate cardiovascular homeostasis. The apelin-APJ pathway may thus provide a mechanism for systemic endothelial monitoring of tissue perfusion and adaptive regulation of cardiovascular function. congestive heart failure; endothelium; gene expression

Published
2008

10. High E-Selectin Ligand Expression Contributes to Chemotherapy-Resistance in Poor Risk Relapsed and Refractory (R/R) Acute Myeloid Leukemia (AML) Patients and Can be Overcome with the Addition of Uproleselan

Author

DeAngelo, Daniel J., primary, Jonas, Brian A, additional, Liesveld, Jane L., additional, Bixby, Dale L., additional, Advani, Anjali S., additional, Marlton, Paula, additional, O'Dwyer, Michael E, additional, Fogler, William E., additional, Magnani, John L., additional, Chen, Mary M, additional, Feldman, Eric J., additional, Thackray, Helen M, additional, and Becker, Pamela S., additional

Published
2019
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11. A Double-Blind, Placebo-Controlled, Phase 3 Registration Trial to Evaluate the Efficacy of Uproleselan (GMI-1271) with Standard Salvage Chemotherapy in Patients with Relapsed/Refractory (R/R) Acute Myeloid Leukemia

Author

DeAngelo, Daniel J., primary, Erba, Harry P., additional, Jonas, Brian A, additional, O'Dwyer, Michael E, additional, Marlton, Paula, additional, Huls, Gerwin, additional, Liesveld, Jane L., additional, Cooper, Brenda, additional, Bhatnagar, Bhavana, additional, Uy, Geoffrey L., additional, Cull, Gavin, additional, Armstrong, Michael B., additional, Fogler, William E., additional, Chen, Mary M, additional, Magnani, John L., additional, Thackray, Helen M, additional, Feldman, Eric J., additional, Advani, Anjali S., additional, and Becker, Pamela S., additional

Published
2019
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15. Pathway analysis of coronary atherosclerosis

Author

King, Jennifer Y., primary, Ferrara, Rossella, additional, Tabibiazar, Raymond, additional, Spin, Joshua M., additional, Chen, Mary M., additional, Kuchinsky, Allan, additional, Vailaya, Aditya, additional, Kincaid, Robert, additional, Tsalenko, Anya, additional, Deng, David Xing-Fei, additional, Connolly, Andrew, additional, Zhang, Peng, additional, Yang, Eugene, additional, Watt, Clifton, additional, Yakhini, Zohar, additional, Ben-Dor, Amir, additional, Adler, Annette, additional, Bruhn, Laurakay, additional, Tsao, Philip, additional, Quertermous, Thomas, additional, and Ashley, Euan A., additional

Published
2005
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18. Novel Role for the Potent Endogenous Inotrope Apelin in Human Cardiac Dysfunction

Author

Chen, Mary M., primary, Ashley, Euan A., additional, Deng, David X.F., additional, Tsalenko, Anya, additional, Deng, Alicia, additional, Tabibiazar, Raymond, additional, Ben-Dor, Amir, additional, Fenster, Brett, additional, Yang, Eugene, additional, King, Jennifer Y., additional, Fowler, Michael, additional, Robbins, Robert, additional, Johnson, Frances L., additional, Bruhn, Laurakay, additional, McDonagh, Theresa, additional, Dargie, Henry, additional, Yakhini, Zohar, additional, Tsao, Philip S., additional, and Quertermous, Thomas, additional

Published
2003
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