Add to ORKGPrevious studies have not completely clarified the precise defect that characterizes B cell development in aged animals. The question of which developmental mechanism is actually deficient in aging remains controversial. The goal of this study was to elucidate the effects of aging on bone marrow B cell population dynamics. We used mathematical modeling to predict the outcome of the different possible effects, and then compared these predictions to experimental data, to find the most plausible effects. Our model shows that the three main differences between B cell development in young and old mice are a decrease in the maximum number of cells in the pre-B compartment and increases in the rate of transition from cycling pre-B cells to resting...
Significant disturbances in B lineage populations of New Zealand Black (NZB) mice have been reported...
Aged humans and experimental animals are impaired in their responses to most foreign antigens althou...
Recent advances allow aging-associated changes in B-cell function to be approached at a mechanistic ...
B cell generation and immunoglobulin (Ig) diversity in mice is compromised with aging. Our recent wo...
B lymphopoiesis in aged mice is characterized by reduced B cell precursors and an altered antibody r...
Advancing age is accompanied by a decrease in the numbers of bone marrow pre-B cells in mice. Using ...
We have described a distinct bone marrow immature B cell population in non-transgenic, adult BALB/c ...
In murine bone marrow, old age (\u3e2 yrs.) is characterized by low production of pre-B and immature...
International audienceAging is associated with a decreased production of B cells by the bone marrow ...
Senescent mice show diminished B lymphopoiesis as well as alterations in mature B cell compartments....
During aging, adaptive immunity is severely compromised, due in part to decreased production of B ly...
We have discovered a distinct mature B-cell subset that accumulates with age, which we have termed a...
To address the fundamental question of whether or not stem cell populations age, we performed quanti...
Senescence in mice is associated with reductions in bone marrow pre-B cells. These follow developmen...
P>Studies in aged mice show that the architecture of B-cell areas appears disrupted and that newly m...
Significant disturbances in B lineage populations of New Zealand Black (NZB) mice have been reported...
Aged humans and experimental animals are impaired in their responses to most foreign antigens althou...
Recent advances allow aging-associated changes in B-cell function to be approached at a mechanistic ...
B cell generation and immunoglobulin (Ig) diversity in mice is compromised with aging. Our recent wo...
B lymphopoiesis in aged mice is characterized by reduced B cell precursors and an altered antibody r...
Advancing age is accompanied by a decrease in the numbers of bone marrow pre-B cells in mice. Using ...
We have described a distinct bone marrow immature B cell population in non-transgenic, adult BALB/c ...
In murine bone marrow, old age (\u3e2 yrs.) is characterized by low production of pre-B and immature...
International audienceAging is associated with a decreased production of B cells by the bone marrow ...
Senescent mice show diminished B lymphopoiesis as well as alterations in mature B cell compartments....
During aging, adaptive immunity is severely compromised, due in part to decreased production of B ly...
We have discovered a distinct mature B-cell subset that accumulates with age, which we have termed a...
To address the fundamental question of whether or not stem cell populations age, we performed quanti...
Senescence in mice is associated with reductions in bone marrow pre-B cells. These follow developmen...
P>Studies in aged mice show that the architecture of B-cell areas appears disrupted and that newly m...
Significant disturbances in B lineage populations of New Zealand Black (NZB) mice have been reported...
Aged humans and experimental animals are impaired in their responses to most foreign antigens althou...
Recent advances allow aging-associated changes in B-cell function to be approached at a mechanistic ...