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69


Assessing the effects of memantine in APP/PS1 transgenic mice by behavioural studies and ex vivo imaging of amyloid plaques using gadolinium labelled amyloid beta peptides and mu MRI [Meeting Abstract]

Scholtzova, H; Wadghiri, YZ; Sigurdsson, EM; Douadi, M; Li, Y; Quartermain, D; Banerjee, PK; Wisniewski, T
ISI:000240771302052
ISSN: 0924-977x
CID: 69190

A-beta derivative vaccine does not cause brain microhemorrhages in Tg2576 mice and its effectiveness is age-dependent [Meeting Abstract]

Boutajangout, Allal; Asuni, Ayodeji A; Scholtzova, Henrieta; Knudsen, Elin; Li, Yong-Shen; Quartermain, David; Frangione, Blas; Wisniewski, Thomas; Sigurdsson, Einar
ORIGINAL:0011722
ISSN: 1552-5279
CID: 2399932

Inhibition the apolipoprotein E/amyloid-beta interaction as a novel therapeutic approach for Alzheimer's disease [Meeting Abstract]

Sadowski, M; Pankiewicz, J; Scholtzova, H; Wen, P; Mehta, P; Quartermain, D; Wisniewski, T
ISI:000236068104254
ISSN: 0028-3878
CID: 97604

Anti-PrP monoclonal antibodies for prevention of prion infection [Meeting Abstract]

Pankiewicz, J; Prelli, F; Sadowski, M; Scholtzova, H; Kascsak, R; Kascsak, R; Carp, RI; Meeker, CH; Sy, MS; Wisniewski, T
ISI:000227841501364
ISSN: 0028-3878
CID: 97606

MRI approaches for specific targeting of PrPSc in the spleen of prion infected presymptomatic subjects [Meeting Abstract]

Sadowski, M; Wadghiri, ZY; Brown, D; Scholtzova, H; Pankiewicz, J; Turnbull, DH; Wisniewski, T
ISI:000227841502409
ISSN: 0028-3878
CID: 97607

Mucosal vaccination delays or prevents prion infection via an oral route

Goni, F; Knudsen, E; Schreiber, F; Scholtzova, H; Pankiewicz, J; Carp, R; Meeker, H C; Rubenstein, R; Brown, D R; Sy, M-S; Chabalgoity, J A; Sigurdsson, E M; Wisniewski, T
In recent years major outbreaks of prion disease linked to oral exposure of the prion agent have occurred in animal and human populations. These disorders are associated with a conformational change of a normal protein, PrP(C) (prion protein cellular), to a toxic and infectious form, PrP(Sc) (prion protein scrapie). None of the prionoses currently have an effective treatment. A limited number of active immunization approaches have been shown to slightly prolong the incubation period of prion infection. Active immunization in wild-type animals is hampered by auto-tolerance to PrP and potential toxicity. Here we report that mucosal vaccination with an attenuated Salmonella vaccine strain expressing the mouse PrP, is effective at overcoming tolerance to PrP and leads to a significant delay or prevention of prion disease in mice later exposed orally to the 139A scrapie strain. This mucosal vaccine induced gut anti-PrP immunoglobulin (Ig)A and systemic anti-PrP IgG. No toxicity was evident with this vaccination approach. This promising finding suggests that mucosal vaccination may be a useful method for overcoming tolerance to PrP and preventing prion infection among animal and potentially human populations at risk
PMID: 15878645
ISSN: 0306-4522
CID: 75837

A Synthetic Peptide Blocking the Apolipoprotein E/{beta}-Amyloid Binding Mitigates {beta}-Amyloid Toxicity and Fibril Formation in Vitro and Reduces {beta}-Amyloid Plaques in Transgenic Mice

Sadowski, Marcin; Pankiewicz, Joanna; Scholtzova, Henrieta; Ripellino, James A; Li, Yongsheng; Schmidt, Stephen D; Mathews, Paul M; Fryer, John D; Holtzman, David M; Sigurdsson, Einar M; Wisniewski, Thomas
Alzheimer's disease (AD) is associated with accumulation of beta-amyloid (Abeta). A major genetic risk factor for sporadic AD is inheritance of the apolipoprotein (apo) E4 allele. ApoE can act as a pathological chaperone of Abeta, promoting its conformational transformation from soluble Abeta into toxic aggregates. We determined if blocking the apoE/Abeta interaction reduces Abeta load in transgenic (Tg) AD mice. The binding site of apoE on Abeta corresponds to residues 12 to 28. To block binding, we synthesized a peptide containing these residues, but substituted valine at position 18 to proline (Abeta12-28P). This changed the peptide's properties, making it non-fibrillogenic and non-toxic. Abeta12-28P competitively blocks binding of full-length Abeta to apoE (IC(50) = 36.7 nmol). Furthermore, Abeta12-28P reduces Abeta fibrillogenesis in the presence of apoE, and Abeta/apoE toxicity in cell culture. Abeta12-28P is blood-brain barrier-permeable and in AD Tg mice inhibits Abeta deposition. Tg mice treated with Abeta12-28P for 1 month had a 63.3% reduction in Abeta load in the cortex (P = 0.0043) and a 59.5% (P = 0.0087) reduction in the hippocampus comparing to age-matched control Tg mice. Antibodies against Abeta were not detected in sera of treated mice; therefore the observed therapeutic effect of Abeta12-28P cannot be attributed to an antibody clearance response. Our experiments demonstrate that compounds blocking the interaction between Abeta and its pathological chaperones may be beneficial for treatment of beta-amyloid deposition in AD
PMCID:1618605
PMID: 15331417
ISSN: 0002-9440
CID: 44511

Blocking the apolipoprotein E/beta-amyloid interaction by synthetic peptide mitigates beta-amyloid toxicity and fibril formation in vitro and in vivo [Meeting Abstract]

Sadowski, M; Pankiewicz, J; Scholtzova, H; Li, Y; Sigurdsson, EM; Wisniewski, T
ISI:000224796100570
ISSN: 0961-8368
CID: 55684

Imaging and therapeutic approaches for beta-sheet structures in prion and Alzheimer's diseases [Meeting Abstract]

Wisniewski, T; Pankiewicz, J; Scholtzova, H; Fernando, G; Chabalgoity, JA; Ji, Y; Wadghiri, YZ; Gan, WB; Tang, CY; Turnbull, DH; Mathis, CA; Kascsak, R; Klunk, WE; Carp, RI; Frangione, B; Sigurdsson, EM; Sadowski, M
ISI:000223058700101
ISSN: 0197-4580
CID: 97595

Age-associated behavioral, metabolic, and structural changes in wild-type littermates of Alzheimer's transgenic mice [Meeting Abstract]

Scholtzova, H; Pankiewicz, J; Sadowski, M; Quartermain, D; Jensen, CH; Duff, K; Nixon, RA; Helpern, JH; Gruen, RJ; Wisniewski, T
ISI:000223058700753
ISSN: 0197-4580
CID: 47726