Passive immunotherapy against Aβ in aged APP-transgenic mice reverses cognitive deficits and depletes parenchymal amyloid deposits in spite of increased vascular amyloid and microhemorrhage
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作者:
Wilcock, Donna M.
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Univ S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USAUniv S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USA
Wilcock, Donna M.
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Rojiani, Amyn
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Univ S Florida, Dept Interdisciplinary Oncol, Alzheimers Res Lab, Tampa, FL 33612 USAUniv S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USA
Rojiani, Amyn
[2
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Rosenthal, Arnon
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Rinat Neurosci Corp, Palo Alto, CA 94304 USAUniv S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USA
Rosenthal, Arnon
[3
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Subbarao, Sangeetha
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Rinat Neurosci Corp, Palo Alto, CA 94304 USAUniv S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USA
Subbarao, Sangeetha
[3
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Freeman, Melissa J.
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Univ S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USAUniv S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USA
Freeman, Melissa J.
[1
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Gordon, Marcia N.
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Univ S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USAUniv S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USA
Gordon, Marcia N.
[1
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Morgan, Dave
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Univ S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USAUniv S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USA
Morgan, Dave
[1
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机构:
[1] Univ S Florida, Dept Pharmacol, Alzheimers Res Lab, Tampa, FL 33612 USA
[2] Univ S Florida, Dept Interdisciplinary Oncol, Alzheimers Res Lab, Tampa, FL 33612 USA
Background: Anti-A beta immunotherapy in transgenic mice reduces both diffuse and compact amyloid deposits, improves memory function and clears early-stage phospho-tau aggregates. As most Alzheimer disease cases occur well past midlife, the current study examined adoptive transfer of anti-A beta antibodies to 19- and 23-month old APP-transgenic mice. Methods: We investigated the effects of weekly anti-A beta antibody treatment on radial-arm water-maze performance, parenchymal and vascular amyloid loads, and the presence of microhemorrhage in the brain. 19-month-old mice were treated for 1, 2 or 3 months while 23-month-old mice were treated for 5 months. Only the 23-month-old mice were subject to radial-arm water-maze testing. Results: After 3 months of weekly injections, this passive immunization protocol completely reversed learning and memory deficits in these mice, a benefit that was undiminished after 5 months of treatment. Dramatic reductions of diffuse A beta immunostaining and parenchymal Congophilic amyloid deposits were observed after five months, indicating that even well-established amyloid deposits are susceptible to immunotherapy. However, cerebral amyloid angiopathy increased substantially with immunotherapy, and some deposits were associated with microhemorrhage. Reanalysis of results collected from an earlier time-course study demonstrated that these increases in vascular deposits were dependent on the duration of immunotherapy. Conclusions: The cognitive benefits of passive immunotherapy persist in spite of the presence of vascular amyloid and small hemorrhages. These data suggest that clinical trials evaluating such treatments will require precautions to minimize potential adverse events associated with microhemorrhage.
机构:
Univ Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, ArgentinaUniv Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, Argentina
Mauriño, J
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Saposnik, G
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Univ Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, ArgentinaUniv Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, Argentina
Saposnik, G
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Lepera, S
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Rey, RC
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Univ Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, ArgentinaUniv Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, Argentina
Rey, RC
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Sica, RE
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Univ Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, ArgentinaUniv Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, Argentina
机构:
Univ Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, ArgentinaUniv Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, Argentina
Mauriño, J
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Saposnik, G
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h-index: 0
机构:
Univ Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, ArgentinaUniv Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, Argentina
Saposnik, G
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机构:
Lepera, S
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Rey, RC
论文数: 0引用数: 0
h-index: 0
机构:
Univ Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, ArgentinaUniv Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, Argentina
Rey, RC
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Sica, RE
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h-index: 0
机构:
Univ Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, ArgentinaUniv Buenos Aires, Hosp JM Ramos Mejia, Dept Neurol, Stroke Serv, RA-1425 Buenos Aires, DF, Argentina