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Sialylation of Prion Protein Controls the Rate of Prion Amplification, the Cross-Species Barrier, the Ratio of PrPSc Glycoform and Prion Infectivity

Figure 4

Influence of PrPC sialylation level on glycoform distribution in PMCAb-derived products.

A. 22L or ME7 brain material was diluted 5×102- or 2×103-fold, respectively, into 10% mouse dsNBH or NBH and subjected to three serial PMCAb rounds with 5-fold dilution between rounds. Prior to electrophoresis samples were treated with PK. Blot was stained with Ab3531 antibody. Undigested 1% mouse NBH was used as a reference. B. Western blot of 22L or ME7 scrapie brain material (SBH) or material produced in PMCAb using NBH or dsNBH (dsPMCAb), and stained with Ab3531 antibody. C. Western blot of 263K or SSLOW scrapie brain material (SBH) or material produced in PMCAb using NBH or dsNBH (dsPMCAb), and stained with 3F4 antibody. Black and white triangles mark di- and mono-glycosylated glycoforms, respectively, whereas arrows mark the unglycosylated form.

Figure 4

doi: https://doi.org/10.1371/journal.ppat.1004366.g004