Osteopontin binds ICOSL promoting tumor metastasis.

Davide Raineri,Chiara Dianzani,Giuseppe Cappellano,Federica Maione,Gianluca Baldanzi,Ilaria Iacobucci,Nausicaa Clemente,Giulia Baldone,Elena Boggio,Casimiro Luca Gigliotti,Renzo Boldorini,José M. Rojo,Maria Chiara Monti,Leila Birolo,Umberto Dianzani,Annalisa Chiocchetti

Osteopontin binds ICOSL promoting tumor metastasis.

2020

Davide Raineri
Chiara Dianzani
Giuseppe Cappellano
Federica Maione
Gianluca Baldanzi
Ilaria Iacobucci
Nausicaa Clemente
Giulia Baldone
Elena Boggio
Casimiro Luca Gigliotti
Renzo Boldorini
José M. Rojo
Maria Chiara Monti
Leila Birolo
Umberto Dianzani
Annalisa Chiocchetti

ICOSL/ICOS are costimulatory molecules pertaining to immune checkpoints; their binding transduces signals having anti-tumor activity. Osteopontin (OPN) is here identified as a ligand for ICOSL. OPN binds a different domain from that used by ICOS, and the binding induces a conformational change in OPN, exposing domains that are relevant for its functions. Here we show that in vitro, ICOSL triggering by OPN induces cell migration, while inhibiting anchorage-independent cell growth. The mouse 4T1 breast cancer model confirms these data. In vivo, OPN-triggering of ICOSL increases angiogenesis and tumor metastatization. The findings shed new light on ICOSL function and indicate that another partner beside ICOS may be involved; they also provide a rationale for developing alternative therapeutic approaches targeting this molecular trio.

Keywords:

In vitro
Cancer research
Osteopontin
Angiogenesis
Metastasis
Immune system
Cell migration
Chemistry
Cell growth
In vivo

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