| Literature DB >> 32931746 |
Xinyu Chen1, Majd M Ariss1, Gopalakrishnan Ramakrishnan1, Veronique Nogueira1, Catherine Blaha1, William Putzbach1, Abul B M M K Islam2, Maxim V Frolov1, Nissim Hay3.
Abstract
Studies in three mouse models of breast cancer identified profound discrepancies between cell-autonomous and systemic Akt1- or Akt2-inducible deletion on breast cancer tumorigenesis and metastasis. Although systemic Akt1 deletion inhibits metastasis, cell-autonomous Akt1 deletion does not. Single-cell mRNA sequencing revealed that systemic Akt1 deletion maintains the pro-metastatic cluster within primary tumors but ablates pro-metastatic neutrophils. Systemic Akt1 deletion inhibits metastasis by impairing survival and mobilization of tumor-associated neutrophils. Importantly, either systemic or neutrophil-specific Akt1 deletion is sufficient to inhibit metastasis of Akt-proficient tumors. Thus, Akt1-specific inhibition could be therapeutic for breast cancer metastasis regardless of primary tumor origin. Systemic Akt2 deletion does not inhibit and exacerbates mammary tumorigenesis and metastasis, but cell-autonomous Akt2 deletion prevents breast cancer tumorigenesis by ErbB2. Elevated circulating insulin level induced by Akt2 systemic deletion hyperactivates tumor Akt, exacerbating ErbB2-mediated tumorigenesis, curbed by pharmacological reduction of the elevated insulin.Entities:
Keywords: Akt1; Akt2; breast cancer; insulin; metastasis; neutrophils; therapy
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Year: 2020 PMID: 32931746 DOI: 10.1016/j.molcel.2020.08.017
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970