Specific cancer-associated mutations in the switch III region of Ras increase tumorigenicity by nanocluster augmentation

Alok Jaiswal; Maja Šolman; Hong Liang; Daniel Abankwa; Harri Härmä; John F Hancock; Tero Aittokallio; Alessio Ligabue; Kari Kopra; Camilo Guzmán; Benoit Lectez; Olga Blaževitš; Yong Zhou

Specific cancer-associated mutations in the switch III region of Ras increase tumorigenicity by nanocluster augmentation

Alok Jaiswal; Maja Šolman; Hong Liang; Daniel Abankwa; Harri Härmä; John F Hancock; Tero Aittokallio; Alessio Ligabue; Kari Kopra; Camilo Guzmán; Benoit Lectez; Olga Blaževitš; Yong Zhou

Specific cancer-associated mutations in the switch III region of Ras increase tumorigenicity by nanocluster augmentation

Alok Jaiswal

Maja Šolman

Hong Liang

Daniel Abankwa

Harri Härmä

John F Hancock

Tero Aittokallio

Alessio Ligabue

Kari Kopra

Camilo Guzmán

Benoit Lectez

Olga Blaževitš

Yong Zhou

Katso/Avaa

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Lataukset:

doi:10.7554/eLife.08905

URI

https://elifesciences.org/articles/08905

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Julkaisun pysyvä osoite on:
https://urn.fi/URN:NBN:fi-fe2021042714263

Tiivistelmä

Hotspot mutations of Ras drive cell transformation and tumorigenesis. Less frequent mutations in Ras are poorly characterized for their oncogenic potential. Yet insight into their mechanism of action may point to novel opportunities to target Ras. Here, we show that several cancer-associated mutations in the switch III region moderately increase Ras activity in all isoforms. Mutants are biochemically inconspicuous, while their clustering into nanoscale signaling complexes on the plasma membrane, termed nanocluster, is augmented. Nanoclustering dictates downstream effector recruitment, MAPK-activity, and tumorigenic cell proliferation. Our results describe an unprecedented mechanism of signaling protein activation in cancer.

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