It has been shown that tumor suppressor genes (eg, p16) have pleiotropic effects during lifetime preventing the formation of cancer during early life but contributing to impairments in stem-cell function and organ maintenance during aging. Liu et al provide the first experimental evidence for lineage-specific pleiotropic effects of p16 in the aging immune system. B lineage–specific deletion of p16 leads to B cell–derived neoplasms in middle-aged mice without improving B lymphopoiesis at this age. In contrast, T lineage–specific deletion of p16 does not lead to tumorigenesis but significantly improves T lymphopoiesis and immune functions in aging mice. The data indicate that p16 does not contribute to tumor suppression in T-lymphoid cells but has an important tumor-suppressive role in B-lymphoid cells. In contrast, p16 contributes to impairments in T lymphopoiesis during aging but has no significant effects on B lymphopoiesis in middle-aged mice. Inhibitory effects of p16 on B lymphopoiesis at advanced age cannot be excluded. The data support a new concept indicating that lineage-specific gene-targeting (targeting of p16 in T-lymphoid lineage) could represent a therapeutic option to improve tissue maintenance during aging (T lymphopoiesis) without affecting gene expression and transformation in other compartments (B-lymphoid lineage).

It has been shown that tumor suppressor genes (eg, p16) have pleiotropic effects during lifetime preventing the formation of cancer during early life but contributing to impairments in stem-cell function and organ maintenance during aging. Liu et al provide the first experimental evidence for lineage-specific pleiotropic effects of p16 in the aging immune system. B lineage–specific deletion of p16 leads to B cell–derived neoplasms in middle-aged mice without improving B lymphopoiesis at this age. In contrast, T lineage–specific deletion of p16 does not lead to tumorigenesis but significantly improves T lymphopoiesis and immune functions in aging mice. The data indicate that p16 does not contribute to tumor suppression in T-lymphoid cells but has an important tumor-suppressive role in B-lymphoid cells. In contrast, p16 contributes to impairments in T lymphopoiesis during aging but has no significant effects on B lymphopoiesis in middle-aged mice. Inhibitory effects of p16 on B lymphopoiesis at advanced age cannot be excluded. The data support a new concept indicating that lineage-specific gene-targeting (targeting of p16 in T-lymphoid lineage) could represent a therapeutic option to improve tissue maintenance during aging (T lymphopoiesis) without affecting gene expression and transformation in other compartments (B-lymphoid lineage).

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