Your search keyword '"Chabner, Karissa T."' showing total 6 results

1. Haematopoietic stem cells depend on Gαs-mediated signalling to engraft bone marrow.

Author

Adams, Gregor B., Alley, Ian R., Chung, Ung-il, Chabner, Karissa T., Jeanson, Nathaniel T., Lo Celso, Cristina, Marsters, Emily S., Chen, Min, Weinstein, Lee S., Lin, Charles P., Kronenberg, Henry M., and Scadden, David T.

Subjects

STEM cell research, BONE grafting, BONE marrow, FETAL development, G proteins, LABORATORY mice, CHEMOTAXIS, CYTOKINES

Abstract

Haematopoietic stem and progenitor cells (HSPCs) change location during development and circulate in mammals throughout life, moving into and out of the bloodstream to engage bone marrow niches in sequential steps of homing, engraftment and retention. Here we show that HSPC engraftment of bone marrow in fetal development is dependent on the guanine-nucleotide-binding protein stimulatory α subunit (Gαs). HSPCs from adult mice deficient in Gαs (Gαs-/-) differentiate and undergo chemotaxis, but also do not home to or engraft in the bone marrow in adult mice and demonstrate a marked inability to engage the marrow microvasculature. If deleted after engraftment, Gαs deficiency did not lead to lack of retention in the marrow, rather cytokine-induced mobilization into the blood was impaired. Testing whether activation of Gαs affects HSPCs, pharmacological activators enhanced homing and engraftment in vivo. Gαs governs specific aspects of HSPC localization under physiological conditions in vivo and may be pharmacologically targeted to improve transplantation efficiency. [ABSTRACT FROM AUTHOR]

Published

2009

2. Therapeutic targeting of a stem cell niche.

Author

Adams, Gregor B., Martin, Roderick P., Alley, Ian R., Chabner, Karissa T., Cohen, Kenneth S., Calvi, Laura M., Kronenberg, Henry M., and Scadden, David T.

Subjects

STEM cell treatment, HEMATOPOIETIC stem cells, PARATHYROID hormone, DRUG therapy, HEMATOPOIESIS, HEMATOPOIETIC growth factors, THERAPEUTICS

Abstract

The specialized microenvironment or niche where stem cells reside provides regulatory input governing stem cell function. We tested the hypothesis that targeting the niche might improve stem cell–based therapies using three mouse models that are relevant to clinical uses of hematopoietic stem (HS) cells. We and others previously identified the osteoblast as a component of the adult HS cell niche and established that activation of the parathyroid hormone (PTH) receptor on osteoblasts increases stem cell number. Here we show that pharmacologic use of PTH increases the number of HS cells mobilized into the peripheral blood for stem cell harvests, protects stem cells from repeated exposure to cytotoxic chemotherapy and expands stem cells in transplant recipients. These data provide evidence that the niche may be an attractive target for drug-based stem cell therapeutics. [ABSTRACT FROM AUTHOR]

Published

2007

3. Stem cell engraftment at the endosteal niche is specified by the calcium-sensing receptor.

Author

Adams, Gregor B., Chabner, Karissa T., Alley, Ian R., Olson, Douglas P., Szczepiorkowski, Zbigniew M., Poznansky, Mark C., Kos, Claudine H., Pollak, Martin R., Brown, Edward M., and Scadden, David T.

Subjects

*STEM cells, *CHROMOSOMAL translocation, *BONE marrow, *HEMATOPOIESIS, *BONES, *CALCIUM ions, *HEMATOPOIETIC system

Abstract

During mammalian ontogeny, haematopoietic stem cells (HSCs) translocate from the fetal liver to the bone marrow, where haematopoiesis occurs throughout adulthood. Unique features of bone that contribute to a microenvironmental niche for stem cells might include the known high concentration of calcium ions at the HSC-enriched endosteal surface. Cells respond to extracellular ionic calcium concentrations through the seven-transmembrane-spanning calcium-sensing receptor (CaR), which we identified as being expressed on HSCs. Here we show that, through the CaR, the simple ionic mineral content of the niche may dictate the preferential localization of adult mammalian haematopoiesis in bone. Antenatal mice deficient in CaR had primitive haematopoietic cells in the circulation and spleen, whereas few were found in bone marrow. CaR-/- HSCs from fetal liver were normal in number, in proliferative and differentiative function, and in migration and homing to the bone marrow. Yet they were highly defective in localizing anatomically to the endosteal niche, behaviour that correlated with defective adhesion to the extracellular matrix protein, collagen I. CaR has a function in retaining HSCs in close physical proximity to the endosteal surface and the regulatory niche components associated with it. [ABSTRACT FROM AUTHOR]

Published

2006

4. Efficient generation of human T cells from a tissue-engineered thymic organoid.

Author

Poznansky, Mark C., Evans, Richard H., Foxall, Russell B., Olszak, Ivona T., Piascik, Anita H., Hartman, Kelly E., Brander, Christian, Meyer, Thomas H., Pykett, Mark J., Chabner, Karissa T., Kalams, Spyros A., Rosenzweig, Michael, and Scadden, David T.

Subjects

T cells, GENETIC engineering, TANTALUM

Abstract

Biocompatible inorganic matrices have been used to enhance bone repair by integrating with endogenous bone architecture. Hypothesizing that a three-dimensional framework might support reconstruction of other tissues as well, we assessed the capacity of a tantalum-coated carbon matrix to support reconstitution of functioning thymic tissue. We engineered a thymic organoid by seeding matrices with murine thymic stroma. Co-culture of human bone marrow-derived hematopoietic progenitor cells within this xenogeneic environment generated mature functional T cells within 14 days. The proportionate T-cell yield from this system was highly reproducible, generating over 70% CD3[SUP+] T cells from either AC133[SUP+] or CD34[SUP+] progenitor cells. Cultured T cells expressed a high level of T-cell receptor excision circles (TREC), demonstrating de novo T lymphopoiesis, and function of fully mature T cells. This system not only facilitates analysis of the T-lymphopoietic potential of progenitor cell populations; it also permits ex vivo genesis of T cells for possible applications in treatment of immunodeficiency. [ABSTRACT FROM AUTHOR]

Published

2000

5. Corrigendum: Therapeutic targeting of a stem cell niche.

Author

Adams, Gregor B., Martin, Roderick P., Alley, Ian R., Chabner, Karissa T., Cohen, Kenneth S., Calvi, Laura M., Kronenberg, Henry M., and Scadden, David T.

Subjects

STEM cell treatment

Abstract

A correction to the article "Therapeutic Targeting of a Stem Cell Niche" that was published in the January 21, 2007 issue is presented.

Published

2008

6. Corrigendum: Therapeutic targeting of a stem cell niche.

Author

Adams, Gregor B, Martin, Roderick P, Alley, Ian R, Chabner, Karissa T, Cohen, Kenneth S, Calvi, Laura M, Kronenberg, Henry M, and Scadden, David T

Subjects

STEM cells

Abstract

This article presents a correction of the January 2007 issue regarding a paper on targeting stem cell niches.

Published

2007