- Autori:
-
Parrasia, Sofia; Paoli, Carlotta; Varanita, Tatiana; Brillo, Valentina; Abdel-Salam, Mostafa A L; Ongaro, Alberto; Hornisch, Claudia; Angi, Beatrice; Bachmann, Magdalena; Bergamin, Filippo; Corbo, Vincenzo; Fiorini, Elena; Rossa, Andrea; Bossio, Giovanna; Gulbins, Erich; Carrer, Alessandro; Zoratti, Mario; Mattarei, Andrea; Ruzza, Paolo; Biasutto, Lucia; Szabo, Ildiko
- Titolo:
-
Tumor-specific targeting of a mitochondrial Kv1.3 channel inhibitor through conjugation to gastrin/cholecystokinin B receptor ligand strongly reduces pancreatic ductal adenocarcinoma in orthotopic models
- Anno:
-
2026
- Tipologia prodotto:
-
Articolo in Rivista
- Tipologia ANVUR:
- Articolo su rivista
- Lingua:
-
Inglese
- Formato:
-
Elettronico
- Referee:
-
No
- Nome rivista:
- Pharmacological Research
- ISSN Rivista:
- 1043-6618
- N° Volume:
-
225
- Intervallo pagine:
-
1-20
- Parole chiave:
-
Kv1.3 channel; mitochondria; pancreatic cancer; tumor-targeting peptides
- Breve descrizione dei contenuti:
- : Pancreatic ductal adenocarcinoma (PDAC) is a highly chemoresistant and immunoresistant tumor with an overall five-year survival rate of less than 10%. Current treatments for PDAC are rather limited, highlighting the importance of finding novel strategies. In this study, we investigated a strategy for the tumor-specific targeting of PAPTP, a small molecule that reduces PDAC growth by inhibiting the mitochondrial potassium channel mtKv1.3, thereby inducing mitochondrial dysfunction and killing cancer cells. PAPTP was reversibly conjugated to three tumor-penetrating peptides: iRGD, VH434, and a short version of minigastrin (CCK2p). These recognize neuropilin-1 and integrin (iRGD), the low-density lipoprotein receptor (VH434), and the gastrin/cholecystokinin B receptor (CCK2p). In vivo pharmacokinetic studies revealed that the PAPTP-bound iRGD peptide underwent rapid metabolic cleavage, which prevented optimal uptake of the construct into PDAC. The VH434 conjugate was highly hemolytic. However, CCK2p-PAPTP exhibited preferential distribution to the pancreas in animals bearing orthotopic PDAC. Efficacy studies revealed a reduction in mean tumor volume of up to 65% in two independent orthotopic mouse models, with no tumor evident in some of the animals treated with the CCK2p-boundPAPTP construct. Our data suggest that tumor-specific targeting of small molecules may be a promising strategy for precision medicine against PDAC.
- Note:
- Available online 20 February 2026
- Id prodotto:
-
150046
- Handle IRIS:
-
11562/1184269
- ultima modifica:
-
15 marzo 2026
- Citazione bibliografica:
-
Parrasia, Sofia; Paoli, Carlotta; Varanita, Tatiana; Brillo, Valentina; Abdel-Salam, Mostafa A L; Ongaro, Alberto; Hornisch, Claudia; Angi, Beatrice; Bachmann, Magdalena; Bergamin, Filippo; Corbo, Vincenzo; Fiorini, Elena; Rossa, Andrea; Bossio, Giovanna; Gulbins, Erich; Carrer, Alessandro; Zoratti, Mario; Mattarei, Andrea; Ruzza, Paolo; Biasutto, Lucia; Szabo, Ildiko,
Tumor-specific targeting of a mitochondrial Kv1.3 channel inhibitor through conjugation to gastrin/cholecystokinin B receptor ligand strongly reduces pancreatic ductal adenocarcinoma in orthotopic models
«Pharmacological Research»
, vol.
225
,
2026
,
pp. 1-20
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