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Dive into the research topics where Andrew BitMansour is active.

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Featured researches published by Andrew BitMansour.


The Journal of Infectious Diseases | 2005

Protection against Lethal Aspergillus fumigatus Infection in Mice by Allogeneic Myeloid Progenitors Is Not Major Histocompatibility Complex Restricted

Caroline Arber; Andrew BitMansour; Sumana Shashidhar; Sophia Y. Wang; Benjamin Tseng; Janice M. Brown

Invasive fungal infections are a leading cause of morbidity and mortality after myelotoxic chemotherapy or radiation exposure. The resulting depletion of myeloid precursors under these conditions appears to be the factor that limits approaches to accelerate immune reconstitution. In a murine model of myeloablation after radiation exposure, we demonstrated that highly purified common myeloid and granulocyte-monocyte progenitors (CMPs/GMPs) accelerated myeloid recovery and, thus, enhanced innate immunity as measured by survival after a lethal challenge with Aspergillus fumigatus. Of greatest significance was the demonstration that the protection afforded by CMPs/GMPs was not major histocompatibility complex restricted. Furthermore, the effect of CMP/GMP cellular therapy was additive with that of liposomal amphotericin B treatment. These observations greatly expand the potential donor pool and, thus, the clinical utility of CMP/GMP cellular therapy in patients with myeloid depletion.


Journal of Immunology | 2005

Stepwise Development of Committed Progenitors in the Bone Marrow That Generate Functional T Cells in the Absence of the Thymus

Marcos E. García-Ojeda; Sussan Dejbakhsh-Jones; Devavani Chatterjea-Matthes; Aditi Mukhopadhyay; Andrew BitMansour; Irving L. Weissman; Janice M. Brown; Samuel Strober

We identified committed T cell progenitors (CTPs) in the mouse bone marrow that have not rearranged the TCRβ gene; express a variety of genes associated with commitment to the T cell lineage, including GATA-3, T cell-specific factor-1, Cβ, and Id2; and show a surface marker pattern (CD44+CD25−CD24+CD5−) that is similar to the earliest T cell progenitors in the thymus. More mature committed intermediate progenitors in the marrow have rearranged the TCR gene loci, express Vα and Vβ genes as well as CD3ε, but do not express surface TCR or CD3 receptors. CTPs, but not progenitors from the thymus, reconstituted the αβ T cells in the lymphoid tissues of athymic nu/nu mice. These reconstituted T cells vigorously secreted IFN-γ after stimulation in vitro, and protected the mice against lethal infection with murine CMV. In conclusion, CTPs in wild-type bone marrow can generate functional T cells via an extrathymic pathway in athymic nu/nu mice.


The Journal of Infectious Diseases | 2002

Prophylactic Administration of Liposomal Amphotericin B Is Superior to Treatment in a Murine Model of Invasive Aspergillosis after Hematopoietic Cell Transplantation

Andrew BitMansour; Janice M. Brown

With use of a novel model of invasive Aspergillus fumigatus, the efficacy of prophylactic versus therapeutic administration of liposomal amphotericin B (L-AmB) was tested in C57BL/6 mice. After lethal irradiation and transplantation of whole bone marrow (d 0), animals were challenged with conidia either intravenously or via nasal instillation on d +3 and divided into 3 groups: group I received 5% dextrose in water throughout the study period; group II received L-AmB, 5 mg/kg, beginning on d +4; and group III received L-AmB, 5 mg/kg on d -4, d -2, d 0, and d +2, then daily starting d +4. Groups I and II did not survive intravenous challenge, whereas group III had a 40% survival rate. After nasal instillation of conidia, the survival was 25%, 35%, and 85% for mice in groups I, II, and III, respectively. These results demonstrate that prophylactic administration of L-AmB increased early survival against lethal challenge with A. fumigatus, compared with therapy instituted after infection.


Blood | 2002

Myeloid progenitors protect against invasive aspergillosis and Pseudomonas aeruginosa infection following hematopoietic stem cell transplantation

Andrew BitMansour; Stacy M. Burns; David Traver; Koichi Akashi; Christopher H. Contag; Irving L. Weissman; Janice M. Brown


Blood | 2003

Common lymphoid progenitors rapidly engraft and protect against lethal murine cytomegalovirus infection after hematopoietic stem cell transplantation

Caroline Arber; Andrew BitMansour; Timothy E. Sparer; John P. Higgins; Edward S. Mocarski; Irving L. Weissman; Judith A. Shizuru; Janice M. Brown


Blood | 2006

Cytomegalovirus MCK-2 controls mobilization and recruitment of myeloid progenitor cells to facilitate dissemination

Satoshi Noda; Shirley A. Aguirre; Andrew BitMansour; Janice M. Brown; Timothy E. Sparer; Jing Huang; Edward S. Mocarski


Blood | 2005

Single infusion of myeloid progenitors reduces death from Aspergillus fumigatus following chemotherapy-induced neutropenia

Andrew BitMansour; Thai M. Cao; Stephanie Chao; Sumana Shashidhar; Janice M. Brown


Archive | 2013

myeloid progenitor cells to facilitate dissemination Cytomegalovirus MCK-2 controls mobilization and recruitment of

Edward S. Mocarski; Satoshi Noda; Shirley A. Aguirre; Andrew BitMansour; Janice M. Brown; Timothy E. Sparer


Archive | 2013

transplantation murine cytomegalovirus infection after hematopoietic stem cell Common lymphoid progenitors rapidly engraft and protect against lethal

L. Weissman; Judith A. Shizuru; Janice M. Brown; Caroline Arber; Andrew BitMansour; Timothy E. Sparer; John P. Higgins; Edward S. Mocarski


Archive | 2013

transplantation Pseudomonas aeruginosa infection following hematopoietic stem cell Myeloid progenitors protect against invasive aspergillosis and

Janice M. Brown; Andrew BitMansour; Stacy M. Burns; David Traver; Koichi Akashi; Irving L

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David Traver

Howard Hughes Medical Institute

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Stephanie Chao

Lucile Packard Children's Hospital

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