p53 deletion impairs clearance of chromosomal-instable stem cells in aging telomere-dysfunctional mice

Y. Begus-Nahrmann; A. Lechel; A.C. Obenauf; K. Nalapareddy; E. Peit; E. Hoffmann; F. Schlaudraff; B. Liss; P. Schirmacher; H. Kestler; E. Danenberg; N. Barker; H.C. Clevers; M.R. Speicher; K.L. Rudolph

p53 deletion impairs clearance of chromosomal-instable stem cells in aging telomere-dysfunctional mice

Translated title of the contribution: p53 deletion impairs clearance of chromosomal-instable stem cells in aging telomere-dysfunctional mice

Y. Begus-Nahrmann, A. Lechel, A.C. Obenauf, K. Nalapareddy, E. Peit, E. Hoffmann, F. Schlaudraff, B. Liss, P. Schirmacher, H. Kestler, E. Danenberg, N. Barker, H.C. Clevers, M.R. Speicher, K.L. Rudolph

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Telomere dysfunction limits the proliferative capacity of human cells and induces organismal aging by activation of p53 and p21 (refs. 1-6). Although deletion of p21 elongates the lifespan of telomere-dysfunctional mice(2), a direct analysis of p53 in telomere-related aging has been hampered by early tumor formation in p53 knockout mice(6). Here we analyzed the functional consequences of conditional p53 deletion(7). Intestinal deletion of p53 shortened the lifespan of telomere-dysfunctional mice without inducing tumor formation. In contrast to p21 deletion, the deletion of p53 impaired the depletion of chromosomal-instable intestinal stem cells in aging telomere-dysfunctional mice. These instable stem cells contributed to epithelial regeneration leading to an accumulation of chromosomal instability, increased apoptosis, altered epithelial cell differentiation and premature intestinal failure. Together, these results provide the first experimental evidence for an organ system in which p53-dependent mechanisms prevent tissue destruction in response to telomere dysfunction by depleting genetically instable stem cells

Translated title of the contribution	p53 deletion impairs clearance of chromosomal-instable stem cells in aging telomere-dysfunctional mice
Original language	Undefined/Unknown
Pages (from-to)	1138-U125
Number of pages	1014
Journal	Nature Genetics
Volume	41
Issue number	10
Publication status	Published - 2009

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Begus-Nahrmann, Y., Lechel, A., Obenauf, A. C., Nalapareddy, K., Peit, E., Hoffmann, E., Schlaudraff, F., Liss, B., Schirmacher, P., Kestler, H., Danenberg, E., Barker, N., Clevers, H. C., Speicher, M. R., & Rudolph, K. L. (2009). p53 deletion impairs clearance of chromosomal-instable stem cells in aging telomere-dysfunctional mice. Nature Genetics, 41(10), 1138-U125.

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title = "p53 deletion impairs clearance of chromosomal-instable stem cells in aging telomere-dysfunctional mice",

abstract = "Telomere dysfunction limits the proliferative capacity of human cells and induces organismal aging by activation of p53 and p21 (refs. 1-6). Although deletion of p21 elongates the lifespan of telomere-dysfunctional mice(2), a direct analysis of p53 in telomere-related aging has been hampered by early tumor formation in p53 knockout mice(6). Here we analyzed the functional consequences of conditional p53 deletion(7). Intestinal deletion of p53 shortened the lifespan of telomere-dysfunctional mice without inducing tumor formation. In contrast to p21 deletion, the deletion of p53 impaired the depletion of chromosomal-instable intestinal stem cells in aging telomere-dysfunctional mice. These instable stem cells contributed to epithelial regeneration leading to an accumulation of chromosomal instability, increased apoptosis, altered epithelial cell differentiation and premature intestinal failure. Together, these results provide the first experimental evidence for an organ system in which p53-dependent mechanisms prevent tissue destruction in response to telomere dysfunction by depleting genetically instable stem cells",

author = "Y. Begus-Nahrmann and A. Lechel and A.C. Obenauf and K. Nalapareddy and E. Peit and E. Hoffmann and F. Schlaudraff and B. Liss and P. Schirmacher and H. Kestler and E. Danenberg and N. Barker and H.C. Clevers and M.R. Speicher and K.L. Rudolph",

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language = "Undefined/Unknown",

volume = "41",

pages = "1138--U125",

journal = "Nature Genetics",

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TY - JOUR

T1 - p53 deletion impairs clearance of chromosomal-instable stem cells in aging telomere-dysfunctional mice

AU - Begus-Nahrmann, Y.

AU - Lechel, A.

AU - Obenauf, A.C.

AU - Nalapareddy, K.

AU - Peit, E.

AU - Hoffmann, E.

AU - Schlaudraff, F.

AU - Liss, B.

AU - Schirmacher, P.

AU - Kestler, H.

AU - Danenberg, E.

AU - Barker, N.

AU - Clevers, H.C.

AU - Speicher, M.R.

AU - Rudolph, K.L.

N1 - J CT

PY - 2009

Y1 - 2009

N2 - Telomere dysfunction limits the proliferative capacity of human cells and induces organismal aging by activation of p53 and p21 (refs. 1-6). Although deletion of p21 elongates the lifespan of telomere-dysfunctional mice(2), a direct analysis of p53 in telomere-related aging has been hampered by early tumor formation in p53 knockout mice(6). Here we analyzed the functional consequences of conditional p53 deletion(7). Intestinal deletion of p53 shortened the lifespan of telomere-dysfunctional mice without inducing tumor formation. In contrast to p21 deletion, the deletion of p53 impaired the depletion of chromosomal-instable intestinal stem cells in aging telomere-dysfunctional mice. These instable stem cells contributed to epithelial regeneration leading to an accumulation of chromosomal instability, increased apoptosis, altered epithelial cell differentiation and premature intestinal failure. Together, these results provide the first experimental evidence for an organ system in which p53-dependent mechanisms prevent tissue destruction in response to telomere dysfunction by depleting genetically instable stem cells

AB - Telomere dysfunction limits the proliferative capacity of human cells and induces organismal aging by activation of p53 and p21 (refs. 1-6). Although deletion of p21 elongates the lifespan of telomere-dysfunctional mice(2), a direct analysis of p53 in telomere-related aging has been hampered by early tumor formation in p53 knockout mice(6). Here we analyzed the functional consequences of conditional p53 deletion(7). Intestinal deletion of p53 shortened the lifespan of telomere-dysfunctional mice without inducing tumor formation. In contrast to p21 deletion, the deletion of p53 impaired the depletion of chromosomal-instable intestinal stem cells in aging telomere-dysfunctional mice. These instable stem cells contributed to epithelial regeneration leading to an accumulation of chromosomal instability, increased apoptosis, altered epithelial cell differentiation and premature intestinal failure. Together, these results provide the first experimental evidence for an organ system in which p53-dependent mechanisms prevent tissue destruction in response to telomere dysfunction by depleting genetically instable stem cells

M3 - Article

SN - 1061-4036

VL - 41

SP - 1138-U125

JO - Nature Genetics

JF - Nature Genetics

IS - 10

ER -

p53 deletion impairs clearance of chromosomal-instable stem cells in aging telomere-dysfunctional mice

Abstract

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