The ageing systemic milieu negatively regulates neurogenesis and cognitive function

Saul A. Villeda; Jian Luo; Kira I. Mosher; Bende Zou; Markus Britschgi; Gregor Bieri; Trisha M. Stan; Nina Fainberg; Zhaoqing Ding; Alexander Eggel; Kurt M. Lucin; Eva Czirr; Jeong Soo Park; Sebastien Couillard-Després; Ludwig Aigner; Ge Li; Elaine R. Peskind; Jeffrey A. Kaye; Joseph F. Quinn; Douglas R. Galasko; Xinmin S. Xie; Thomas A. Rando; Tony Wyss-Coray

doi:10.1038/nature10357

The ageing systemic milieu negatively regulates neurogenesis and cognitive function

Saul A. Villeda, Jian Luo, Kira I. Mosher, Bende Zou, Markus Britschgi, Gregor Bieri, Trisha M. Stan, Nina Fainberg, Zhaoqing Ding, Alexander Eggel, Kurt M. Lucin, Eva Czirr, Jeong Soo Park, Sebastien Couillard-Després, Ludwig Aigner, Ge Li, Elaine R. Peskind, Jeffrey A. Kaye, Joseph F. Quinn, Douglas R. GalaskoXinmin S. Xie, Thomas A. Rando, Tony Wyss-Coray

Neurology

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1306 Scopus citations

Abstract

In the central nervous system, ageing results in a precipitous decline in adult neural stem/progenitor cells and neurogenesis, with concomitant impairments in cognitive functions. Interestingly, such impairments can be ameliorated through systemic perturbations such as exercise. Here, using heterochronic parabiosis we show that blood-borne factors present in the systemic milieu can inhibit or promote adult neurogenesis in an age-dependent fashion in mice. Accordingly, exposing a young mouse to an old systemic environment or to plasma from old mice decreased synaptic plasticity, and impaired contextual fear conditioning and spatial learning and memory. We identify chemokines-including CCL11 (also known as eotaxin)-the plasma levels of which correlate with reduced neurogenesis in heterochronic parabionts and aged mice, and the levels of which are increased in the plasma and cerebrospinal fluid of healthy ageing humans. Lastly, increasing peripheral CCL11 chemokine levels in vivo in young mice decreased adult neurogenesis and impaired learning and memory. Together our data indicate that the decline in neurogenesis and cognitive impairments observed during ageing can be in part attributed to changes in blood-borne factors.

Original language	English (US)
Pages (from-to)	90-96
Number of pages	7
Journal	Nature
Volume	477
Issue number	7362
DOIs	https://doi.org/10.1038/nature10357
State	Published - Sep 1 2011

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Villeda, S. A., Luo, J., Mosher, K. I., Zou, B., Britschgi, M., Bieri, G., Stan, T. M., Fainberg, N., Ding, Z., Eggel, A., Lucin, K. M., Czirr, E., Park, J. S., Couillard-Després, S., Aigner, L., Li, G., Peskind, E. R., Kaye, J. A., Quinn, J. F., ... Wyss-Coray, T. (2011). The ageing systemic milieu negatively regulates neurogenesis and cognitive function. Nature, 477(7362), 90-96. https://doi.org/10.1038/nature10357

Villeda, SA, Luo, J, Mosher, KI, Zou, B, Britschgi, M, Bieri, G, Stan, TM, Fainberg, N, Ding, Z, Eggel, A, Lucin, KM, Czirr, E, Park, JS, Couillard-Després, S, Aigner, L, Li, G, Peskind, ER, Kaye, JA , Quinn, JF, Galasko, DR, Xie, XS, Rando, TA & Wyss-Coray, T 2011, 'The ageing systemic milieu negatively regulates neurogenesis and cognitive function', Nature, vol. 477, no. 7362, pp. 90-96. https://doi.org/10.1038/nature10357

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title = "The ageing systemic milieu negatively regulates neurogenesis and cognitive function",

abstract = "In the central nervous system, ageing results in a precipitous decline in adult neural stem/progenitor cells and neurogenesis, with concomitant impairments in cognitive functions. Interestingly, such impairments can be ameliorated through systemic perturbations such as exercise. Here, using heterochronic parabiosis we show that blood-borne factors present in the systemic milieu can inhibit or promote adult neurogenesis in an age-dependent fashion in mice. Accordingly, exposing a young mouse to an old systemic environment or to plasma from old mice decreased synaptic plasticity, and impaired contextual fear conditioning and spatial learning and memory. We identify chemokines-including CCL11 (also known as eotaxin)-the plasma levels of which correlate with reduced neurogenesis in heterochronic parabionts and aged mice, and the levels of which are increased in the plasma and cerebrospinal fluid of healthy ageing humans. Lastly, increasing peripheral CCL11 chemokine levels in vivo in young mice decreased adult neurogenesis and impaired learning and memory. Together our data indicate that the decline in neurogenesis and cognitive impairments observed during ageing can be in part attributed to changes in blood-borne factors.",

author = "Villeda, {Saul A.} and Jian Luo and Mosher, {Kira I.} and Bende Zou and Markus Britschgi and Gregor Bieri and Stan, {Trisha M.} and Nina Fainberg and Zhaoqing Ding and Alexander Eggel and Lucin, {Kurt M.} and Eva Czirr and Park, {Jeong Soo} and Sebastien Couillard-Despr{\'e}s and Ludwig Aigner and Ge Li and Peskind, {Elaine R.} and Kaye, {Jeffrey A.} and Quinn, {Joseph F.} and Galasko, {Douglas R.} and Xie, {Xinmin S.} and Rando, {Thomas A.} and Tony Wyss-Coray",

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AU - Luo, Jian

AU - Mosher, Kira I.

AU - Zou, Bende

AU - Britschgi, Markus

AU - Bieri, Gregor

AU - Stan, Trisha M.

AU - Fainberg, Nina

AU - Ding, Zhaoqing

AU - Eggel, Alexander

AU - Lucin, Kurt M.

AU - Czirr, Eva

AU - Park, Jeong Soo

AU - Couillard-Després, Sebastien

AU - Aigner, Ludwig

AU - Li, Ge

AU - Peskind, Elaine R.

AU - Kaye, Jeffrey A.

AU - Quinn, Joseph F.

AU - Galasko, Douglas R.

AU - Xie, Xinmin S.

AU - Rando, Thomas A.

AU - Wyss-Coray, Tony

PY - 2011/9/1

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N2 - In the central nervous system, ageing results in a precipitous decline in adult neural stem/progenitor cells and neurogenesis, with concomitant impairments in cognitive functions. Interestingly, such impairments can be ameliorated through systemic perturbations such as exercise. Here, using heterochronic parabiosis we show that blood-borne factors present in the systemic milieu can inhibit or promote adult neurogenesis in an age-dependent fashion in mice. Accordingly, exposing a young mouse to an old systemic environment or to plasma from old mice decreased synaptic plasticity, and impaired contextual fear conditioning and spatial learning and memory. We identify chemokines-including CCL11 (also known as eotaxin)-the plasma levels of which correlate with reduced neurogenesis in heterochronic parabionts and aged mice, and the levels of which are increased in the plasma and cerebrospinal fluid of healthy ageing humans. Lastly, increasing peripheral CCL11 chemokine levels in vivo in young mice decreased adult neurogenesis and impaired learning and memory. Together our data indicate that the decline in neurogenesis and cognitive impairments observed during ageing can be in part attributed to changes in blood-borne factors.

AB - In the central nervous system, ageing results in a precipitous decline in adult neural stem/progenitor cells and neurogenesis, with concomitant impairments in cognitive functions. Interestingly, such impairments can be ameliorated through systemic perturbations such as exercise. Here, using heterochronic parabiosis we show that blood-borne factors present in the systemic milieu can inhibit or promote adult neurogenesis in an age-dependent fashion in mice. Accordingly, exposing a young mouse to an old systemic environment or to plasma from old mice decreased synaptic plasticity, and impaired contextual fear conditioning and spatial learning and memory. We identify chemokines-including CCL11 (also known as eotaxin)-the plasma levels of which correlate with reduced neurogenesis in heterochronic parabionts and aged mice, and the levels of which are increased in the plasma and cerebrospinal fluid of healthy ageing humans. Lastly, increasing peripheral CCL11 chemokine levels in vivo in young mice decreased adult neurogenesis and impaired learning and memory. Together our data indicate that the decline in neurogenesis and cognitive impairments observed during ageing can be in part attributed to changes in blood-borne factors.

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The ageing systemic milieu negatively regulates neurogenesis and cognitive function

Abstract

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