Background: Pancreatic ductal adenocarcinoma (PDAC) is one of the leading cause of cancer death worldwide. PDACs are characterized by centrosome aberrations, but whether centrosome-related genes influence patient outcomes has not been tested. Methods: Publicly available RNA-sequencing data of patients diagnosed with PDAC were interrogated with unsupervised approaches to identify centrosome protein-encoding genes with prognostic relevance. Candidate genes were validated by immunohistochemistry and multiplex immunofluorescence in a set of clinical PDAC and normal pancreatic tissues. Results: Results showed that two genes CEP250 and CEP170, involved in centrosome linker and centriolar subdistal appendages, were expressed at high levels in PDAC tissues and were correlated with prognosis of PDAC patients in independent databases. Large clustered g-tubulin-labelled centrosomes were linked together by aberrant circular and planarshaped CEP250 arrangements in CEP250-high expressing PDACs. Furthermore, PDACs displayed prominent centrosome separation and reduced CEP164-centrosomal labelling associated with acetylatedtubulin staining compared to normal pancreatic tissues. Interestingly, in a small validation cohort, CEP250-high expressing patients had shorter disease free- and overall-survival and almost none of those who received gemcitabine plus nab-paclitaxel first-line therapy achieved a clinical response. In contrast, weak CEP250 expression was associated with long-term survivors or responses to medical treatments. Conclusions: Alteration of the centriolar cohesion and appendages has effect on the survival of patients with PDAC.

Altered centriolar cohesion by CEP250 and appendages impact outcome of patients with pancreatic cancer / Giordano, G; Cipolletta, G; Mellone, A; Puopolo, G; Coppola, L; De Santis, E; Forte, N; Napolitano, F; Caruso, Fp; Parente, P; Landriscina, M; Cerulo, L; Costa, Mc; Pancione, M.. - In: PANCREATOLOGY. - ISSN 1424-3903. - (2024), pp. 1-10. [10.1016/j.pan.2024.06.010]

Altered centriolar cohesion by CEP250 and appendages impact outcome of patients with pancreatic cancer

Mellone A;De Santis E;Parente P;
2024

Abstract

Background: Pancreatic ductal adenocarcinoma (PDAC) is one of the leading cause of cancer death worldwide. PDACs are characterized by centrosome aberrations, but whether centrosome-related genes influence patient outcomes has not been tested. Methods: Publicly available RNA-sequencing data of patients diagnosed with PDAC were interrogated with unsupervised approaches to identify centrosome protein-encoding genes with prognostic relevance. Candidate genes were validated by immunohistochemistry and multiplex immunofluorescence in a set of clinical PDAC and normal pancreatic tissues. Results: Results showed that two genes CEP250 and CEP170, involved in centrosome linker and centriolar subdistal appendages, were expressed at high levels in PDAC tissues and were correlated with prognosis of PDAC patients in independent databases. Large clustered g-tubulin-labelled centrosomes were linked together by aberrant circular and planarshaped CEP250 arrangements in CEP250-high expressing PDACs. Furthermore, PDACs displayed prominent centrosome separation and reduced CEP164-centrosomal labelling associated with acetylatedtubulin staining compared to normal pancreatic tissues. Interestingly, in a small validation cohort, CEP250-high expressing patients had shorter disease free- and overall-survival and almost none of those who received gemcitabine plus nab-paclitaxel first-line therapy achieved a clinical response. In contrast, weak CEP250 expression was associated with long-term survivors or responses to medical treatments. Conclusions: Alteration of the centriolar cohesion and appendages has effect on the survival of patients with PDAC.
2024
CEP164; CEP170; CEP250; centrosome linker; centriolar appendages; pancreatic ductal adenocarcinoma
01 Pubblicazione su rivista::01a Articolo in rivista
Altered centriolar cohesion by CEP250 and appendages impact outcome of patients with pancreatic cancer / Giordano, G; Cipolletta, G; Mellone, A; Puopolo, G; Coppola, L; De Santis, E; Forte, N; Napolitano, F; Caruso, Fp; Parente, P; Landriscina, M; Cerulo, L; Costa, Mc; Pancione, M.. - In: PANCREATOLOGY. - ISSN 1424-3903. - (2024), pp. 1-10. [10.1016/j.pan.2024.06.010]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1716548
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