Gerstmann-straussler-scheinker disease (Prnp p102l): Amyloid deposits are best recognized by antibodies directed to epitopes in prp region 90-165

Pedro Piccardo; Bernardino Ghetti; Dennis W. Dickson; Harry V. Vinters; Giorgio Giaccone; Orso Bugiani; Fabrizio Tagliavini; Katherine Young; Stephen R. Dlouhy; Charles Seiler; Carrie K. Jones; Alice Lazzarini; Lawrence I. Golbe; Thomas R. Zimmerman; Susan L. Perlman; Donald C. McLachlan; Peter H St George-Hyslop; Anne Lennox

Gerstmann-straussler-scheinker disease (Prnp p102l): Amyloid deposits are best recognized by antibodies directed to epitopes in prp region 90-165

Pedro Piccardo, Bernardino Ghetti, Dennis W. Dickson, Harry V. Vinters, Giorgio Giaccone, Orso Bugiani, Fabrizio Tagliavini, Katherine Young, Stephen R. Dlouhy, Charles Seiler, Carrie K. Jones, Alice Lazzarini, Lawrence I. Golbe, Thomas R. Zimmerman, Susan L. Perlman, Donald C. McLachlan, Peter H St George-Hyslop, Anne Lennox

Fondazione IRCCS Istituto Neurologico "C. Besta"

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

Abstract

Gerstmann-Straussler-Scheinker (GSS) disease is a familial neurological disorder pathologically characterized by accumulation of prion protein (PrP) in the form of fibrillary and non-fibrillary deposits within the cerebrum and cerebellum. We have studied two patients in whom the disease is caused by a leucine for proline amino acid substitution at residue 102 of PrP. In both patients, the neuropathologic findings are similar, consisting of spongiform changes, amyloid deposits, and gliosis. To investigate the antigenic profile of PrP deposits, we used antibodies raised against several peptides that correspond to segments of the N-terminus, repeat region, midregion, and C-terminus of PrP. By immunohistochemistry, PrP amyloid cores are best labeled by antibodies directed to epitopes spanning PrP residues 90-165. In GSS disease caused by a substitution of thymine to cytosine at PRNP codon 198 (Indiana kindred), the major amyloidogenic peptide spans residues 58-150; therefore, in these two genetic forms of GSS disease, amyloid may be composed of different peptides. 1995 by the American Association of Neuropathologists.

Original language	English
Pages (from-to)	790-801
Number of pages	12
Journal	Journal of Neuropathology and Experimental Neurology
Volume	54
Issue number	6
Publication status	Published - 1995

Keywords

Amyloid
Antibodies
Gerstmann-Straussler-Scheinker disease
Immunohistochemistry
Prion protein (PrP)
PrP peptides

ASJC Scopus subject areas

Clinical Neurology
Pathology and Forensic Medicine
Cellular and Molecular Neuroscience
Neurology
Neuroscience(all)

Cite this

Piccardo, P., Ghetti, B., Dickson, D. W., Vinters, H. V., Giaccone, G., Bugiani, O., Tagliavini, F., Young, K., Dlouhy, S. R., Seiler, C., Jones, C. K., Lazzarini, A., Golbe, L. I., Zimmerman, T. R., Perlman, S. L., McLachlan, D. C., George-Hyslop, P. H. S., & Lennox, A. (1995). Gerstmann-straussler-scheinker disease (Prnp p102l): Amyloid deposits are best recognized by antibodies directed to epitopes in prp region 90-165. Journal of Neuropathology and Experimental Neurology, 54(6), 790-801.

Gerstmann-straussler-scheinker disease (Prnp p102l) : Amyloid deposits are best recognized by antibodies directed to epitopes in prp region 90-165. / Piccardo, Pedro; Ghetti, Bernardino; Dickson, Dennis W. et al.

In: Journal of Neuropathology and Experimental Neurology, Vol. 54, No. 6, 1995, p. 790-801.

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

Piccardo, P, Ghetti, B, Dickson, DW, Vinters, HV, Giaccone, G, Bugiani, O, Tagliavini, F, Young, K, Dlouhy, SR, Seiler, C, Jones, CK, Lazzarini, A, Golbe, LI, Zimmerman, TR, Perlman, SL, McLachlan, DC, George-Hyslop, PHS & Lennox, A 1995, 'Gerstmann-straussler-scheinker disease (Prnp p102l): Amyloid deposits are best recognized by antibodies directed to epitopes in prp region 90-165', Journal of Neuropathology and Experimental Neurology, vol. 54, no. 6, pp. 790-801.

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abstract = "Gerstmann-Straussler-Scheinker (GSS) disease is a familial neurological disorder pathologically characterized by accumulation of prion protein (PrP) in the form of fibrillary and non-fibrillary deposits within the cerebrum and cerebellum. We have studied two patients in whom the disease is caused by a leucine for proline amino acid substitution at residue 102 of PrP. In both patients, the neuropathologic findings are similar, consisting of spongiform changes, amyloid deposits, and gliosis. To investigate the antigenic profile of PrP deposits, we used antibodies raised against several peptides that correspond to segments of the N-terminus, repeat region, midregion, and C-terminus of PrP. By immunohistochemistry, PrP amyloid cores are best labeled by antibodies directed to epitopes spanning PrP residues 90-165. In GSS disease caused by a substitution of thymine to cytosine at PRNP codon 198 (Indiana kindred), the major amyloidogenic peptide spans residues 58-150; therefore, in these two genetic forms of GSS disease, amyloid may be composed of different peptides. 1995 by the American Association of Neuropathologists.",

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AU - Piccardo, Pedro

AU - Ghetti, Bernardino

AU - Dickson, Dennis W.

AU - Vinters, Harry V.

AU - Giaccone, Giorgio

AU - Bugiani, Orso

AU - Tagliavini, Fabrizio

AU - Young, Katherine

AU - Dlouhy, Stephen R.

AU - Seiler, Charles

AU - Jones, Carrie K.

AU - Lazzarini, Alice

AU - Golbe, Lawrence I.

AU - Zimmerman, Thomas R.

AU - Perlman, Susan L.

AU - McLachlan, Donald C.

AU - George-Hyslop, Peter H St

AU - Lennox, Anne

PY - 1995

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N2 - Gerstmann-Straussler-Scheinker (GSS) disease is a familial neurological disorder pathologically characterized by accumulation of prion protein (PrP) in the form of fibrillary and non-fibrillary deposits within the cerebrum and cerebellum. We have studied two patients in whom the disease is caused by a leucine for proline amino acid substitution at residue 102 of PrP. In both patients, the neuropathologic findings are similar, consisting of spongiform changes, amyloid deposits, and gliosis. To investigate the antigenic profile of PrP deposits, we used antibodies raised against several peptides that correspond to segments of the N-terminus, repeat region, midregion, and C-terminus of PrP. By immunohistochemistry, PrP amyloid cores are best labeled by antibodies directed to epitopes spanning PrP residues 90-165. In GSS disease caused by a substitution of thymine to cytosine at PRNP codon 198 (Indiana kindred), the major amyloidogenic peptide spans residues 58-150; therefore, in these two genetic forms of GSS disease, amyloid may be composed of different peptides. 1995 by the American Association of Neuropathologists.

AB - Gerstmann-Straussler-Scheinker (GSS) disease is a familial neurological disorder pathologically characterized by accumulation of prion protein (PrP) in the form of fibrillary and non-fibrillary deposits within the cerebrum and cerebellum. We have studied two patients in whom the disease is caused by a leucine for proline amino acid substitution at residue 102 of PrP. In both patients, the neuropathologic findings are similar, consisting of spongiform changes, amyloid deposits, and gliosis. To investigate the antigenic profile of PrP deposits, we used antibodies raised against several peptides that correspond to segments of the N-terminus, repeat region, midregion, and C-terminus of PrP. By immunohistochemistry, PrP amyloid cores are best labeled by antibodies directed to epitopes spanning PrP residues 90-165. In GSS disease caused by a substitution of thymine to cytosine at PRNP codon 198 (Indiana kindred), the major amyloidogenic peptide spans residues 58-150; therefore, in these two genetic forms of GSS disease, amyloid may be composed of different peptides. 1995 by the American Association of Neuropathologists.

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KW - Antibodies

KW - Gerstmann-Straussler-Scheinker disease

KW - Immunohistochemistry

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Gerstmann-straussler-scheinker disease (Prnp p102l): Amyloid deposits are best recognized by antibodies directed to epitopes in prp region 90-165

Abstract

Keywords

ASJC Scopus subject areas

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