Phenotypic Variability of Gerstmann-Straussler-Scheinker Disease is Associated with Prion Protein Heterogeneity

Abstract: Gerstmann-Sträussler-Scheinker disease (GSS), a cerebello-pyramidal syndrome associated with dementia and caused by mutations in the prion protein gene (PRNP), is phenotypically heterogeneous. The molecular mechanisms responsible for such heterogeneity are unknown. Since we hypothesize that prion protein (PrP) heterogeneity may be associated with clinico-pathologic heterogeneity, the aim of this study was to analyze PrP in several GSS variants. Among the pathologic phenotypes of GSS, we recognize those without… Show more

“…It is important to note that the amount of PrP sc in the patients (1 to 5) reported here is significantly smaller than that found in other GSS variants. 11,13 In agreement with the results presented here, recent studies in an Alsatian patient with GSS A117V 18 showed that the major component of amyloid fibrils was a ϳ7-kd peptide with ragged N terminus starting mainly at G 88 and G 90 . 18 The 14-and 7-kd bands, seen in GSS A117V (1 to 5), are detected by antibodies directed to the mid-region of PrP indicating that these fragments include the intact epitope recognized by mAb 3F4 consisting of residues 109 to 112.…”

“…3 GSS is caused by mutations P102L, P105L, A117V, G131V, F198S, D202N, Q212P, and Q217R in PRNP. 3,11,12 The pathological hallmark of GSS is the accumulation of PrP, with and without amyloid tinctorial properties, in the brain. 3 Our studies have shown that the pattern of PrP sc isoforms in the multiple GSS variants analyzed is different from that seen in CJD.…”

“…3 Our studies have shown that the pattern of PrP sc isoforms in the multiple GSS variants analyzed is different from that seen in CJD. [11][12][13] Patients with CJD present full-length and Ntruncated PrP fragments whereas patients with GSS present full-length as well as N-and C-terminal truncated PrP peptides. 10 -13,14,15 Previous studies showed that the amyloid subunit in GSS F198S is a 7-kd peptide with an N terminus at residue G 81 .…”

“…13 In GSS A117V, previous studies have been contradictory in terms of whether or not PK-resistant PrP is present. 11,19,20 The aims of the present study are to determine the biochemical characteristics of PrP in several patients and an asymptomatic carrier from two unrelated American families with PRNP A117V. 21,22 We analyzed brain homogenates, microsomal preparations, and purified PrP fractions.…”

“…Samples were resolved in 4 to 12% acrylamide gels and transferred to nitrocellulose membranes as described. 11,13 Membranes were probed with monoclonal antibody (mAb) 3F4. 27 Immunoblot analysis for PrP sc was done after digestion of the homogenates with PK (10 g/ml) for 1 hour at 37°C.…”

Prion Proteins with Different Conformations Accumulate in Gerstmann-Sträussler-Scheinker Disease Caused by A117V and F198S Mutations

“…It is important to note that the amount of PrP sc in the patients (1 to 5) reported here is significantly smaller than that found in other GSS variants. 11,13 In agreement with the results presented here, recent studies in an Alsatian patient with GSS A117V 18 showed that the major component of amyloid fibrils was a ϳ7-kd peptide with ragged N terminus starting mainly at G 88 and G 90 . 18 The 14-and 7-kd bands, seen in GSS A117V (1 to 5), are detected by antibodies directed to the mid-region of PrP indicating that these fragments include the intact epitope recognized by mAb 3F4 consisting of residues 109 to 112.…”

“…3 GSS is caused by mutations P102L, P105L, A117V, G131V, F198S, D202N, Q212P, and Q217R in PRNP. 3,11,12 The pathological hallmark of GSS is the accumulation of PrP, with and without amyloid tinctorial properties, in the brain. 3 Our studies have shown that the pattern of PrP sc isoforms in the multiple GSS variants analyzed is different from that seen in CJD.…”

“…3 Our studies have shown that the pattern of PrP sc isoforms in the multiple GSS variants analyzed is different from that seen in CJD. [11][12][13] Patients with CJD present full-length and Ntruncated PrP fragments whereas patients with GSS present full-length as well as N-and C-terminal truncated PrP peptides. 10 -13,14,15 Previous studies showed that the amyloid subunit in GSS F198S is a 7-kd peptide with an N terminus at residue G 81 .…”

“…13 In GSS A117V, previous studies have been contradictory in terms of whether or not PK-resistant PrP is present. 11,19,20 The aims of the present study are to determine the biochemical characteristics of PrP in several patients and an asymptomatic carrier from two unrelated American families with PRNP A117V. 21,22 We analyzed brain homogenates, microsomal preparations, and purified PrP fractions.…”

“…Samples were resolved in 4 to 12% acrylamide gels and transferred to nitrocellulose membranes as described. 11,13 Membranes were probed with monoclonal antibody (mAb) 3F4. 27 Immunoblot analysis for PrP sc was done after digestion of the homogenates with PK (10 g/ml) for 1 hour at 37°C.…”

Prion Proteins with Different Conformations Accumulate in Gerstmann-Sträussler-Scheinker Disease Caused by A117V and F198S Mutations

A New PRNP Mutation (G131V) Associated With Gerstmann-Sträussler-Scheinker Disease

Unusual Clinical and Molecular-Pathological Profile of Gerstmann-Sträussler-Scheinker Disease Associated With a NovelPRNPMutation (V176G)