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Pichia pastoris as a host for secretion of toxic Saporin chimaeras

Articolo
Data di Pubblicazione:
2010
Abstract:
Most of the targeting moieties such as antibody fragments or growth factor domains used to construct targeted toxins for anticancer therapy derive from secretory proteins. These normally fold in the oxidative environment of the endoplasmic reticulum (ER) and hence their folding in bacterial cells can be quite inefficient. For instance, only low amounts of properly folded antimetastatic chimaera constituted by the Amino-Terminal Fragment of human urokinase (ATF) fused to the plant ribosome-inactivating protein Saporin could be recovered. ATF-saporin was instead secreted efficiently when expressed in eukaryotic cells protected from autointoxication with neutralizing anti-Saporin antibodies. Pichia pastoris is a microbial eukaryotic host where these domains can fold into a transport-competent conformation and reach the extracellular medium. We show here that despite some host toxicity, codon-usage optimization greatly increased the expression levels of active Saporin but not those of an active-site mutant SAP-KQ in GS115 (his4) strain. The lack of any toxicity associated with expression of the latter confirmed that toxicity is due to Saporin catalytic activity. Nevertheless, GS115 (his4) cells in flask culture secreted 3.5mg/L of a histidine-tagged ATF-saporin chimaera showing IC50 6x10-11M against U937 cells, thus demonstrating the suitability of this expression platform for secretion of toxic Saporin-based chimaeras.
Tipologia CRIS:
01.01 Articolo in rivista
Keywords:
codon-usage; eukaryotic expression; human urokinase receptor; plant ribosome-inactivating proteins; tumor-targeted therapy
Elenco autori:
Lombardi, Alessio; Fabbrini, MARIA SERENA; Bursomanno, Sara; Ceriotti, Aldo
Autori di Ateneo:
CERIOTTI ALDO
Link alla scheda completa:
https://iris.cnr.it/handle/20.500.14243/160384
Pubblicato in:
THE FASEB JOURNAL
Journal
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