Figure 1
Figure 1. Maturation and processing of HJV. (A) Schematic representation of HJV functional domains and localization of the studied mutations. SP indicates signal peptide; RGD, arginine-glycine–aspartic acid integrin-binding domain; ⋄, Cys residue; and •, Asn residue. The dotted line indicates the autoproteolytic site. The double line shows the peptide chosen for antibody production. (B) Characterization of the mouse polyclonal anti-HJV. Hela cells were transfected with empty vector (mock) or WT HJV-expressing construct (WT). HJV was synthesized by in vitro transcription and translation (TNT). *Unspecific band. Anti-HJV recognizes a major band, which corresponds to the mature HJV, and a faint band derived from the autoproteolysis of the VWF type D domain. (C-D) WT and mutants HJV (30 μg of total lysates) were treated (+) with Endo H (C) or PNGase F (D) following manufacturer's instructions. (E) The nonsense R326X mutation produces a truncated HJV that is partially glycosylated, as shown by the band shift after Endo H and PNGase F treatment. The arrows show the glycosylation state. Scales refer to relative molecular mass in kilodaltons.

Maturation and processing of HJV. (A) Schematic representation of HJV functional domains and localization of the studied mutations. SP indicates signal peptide; RGD, arginine-glycine–aspartic acid integrin-binding domain; ⋄, Cys residue; and •, Asn residue. The dotted line indicates the autoproteolytic site. The double line shows the peptide chosen for antibody production. (B) Characterization of the mouse polyclonal anti-HJV. Hela cells were transfected with empty vector (mock) or WT HJV-expressing construct (WT). HJV was synthesized by in vitro transcription and translation (TNT). *Unspecific band. Anti-HJV recognizes a major band, which corresponds to the mature HJV, and a faint band derived from the autoproteolysis of the VWF type D domain. (C-D) WT and mutants HJV (30 μg of total lysates) were treated (+) with Endo H (C) or PNGase F (D) following manufacturer's instructions. (E) The nonsense R326X mutation produces a truncated HJV that is partially glycosylated, as shown by the band shift after Endo H and PNGase F treatment. The arrows show the glycosylation state. Scales refer to relative molecular mass in kilodaltons.

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