Citation

  • Authors: Pereira PMR. et al.
  • Year: 2022
  • Journal: Nat Commun 13 2526
  • Applications: in vitro / DNA / jetPRIME
  • Cell type: HEK-293T
    Description: Human embryonic kidney Fibroblast
    Known as: HEK293T, 293T

Method

Lentivirus was produced by transfection of HEK293T cells using the JetPrime system (Polyplus). The ratio of pMD2.G:psPAX2:pHAGE-ERBB2 was 1:2:3, the ratio of JetPrime transfection reagent to DNA was 2:1, and the ratio of JetPrime buffer:transfection reagent was 50:1. The HEK293T cells were incubated with the DNA and transfection reagents for 24 h before the media was changed. Two days after replacing the media, the media (herein referred to as viral supernatant) was collected and filtered through 0.45 μM PVDF filters (Millipore). The viral supernatant was then concentrated 20-fold with Lenti-X Concentrator (Clontech) according to the manufacturer’s instructions.

Abstract

Resistance mechanisms and heterogeneity in HER2-positive gastric cancers (GC) limit Trastuzumab benefit in 32% of patients, and other targeted therapies have failed in clinical trials. Using patient samples, patient-derived xenografts (PDXs), partially humanized biological models, and HER2-targeted imaging technologies we demonstrate the role of caveolin-1 (CAV1) as a complementary biomarker in GC selection for Trastuzumab therapy. In retrospective analyses of samples from patients enrolled on Trastuzumab trials, the CAV1-high profile associates with low membrane HER2 density and low patient survival. We show a negative correlation between CAV1 tumoral protein levels - a major protein of cholesterol-rich membrane domains - and Trastuzumab-drug conjugate TDM1 tumor uptake. Finally, CAV1 depletion using knockdown or pharmacologic approaches (statins) increases antibody drug efficacy in tumors with incomplete HER2 membranous reactivity. In support of these findings, background statin use in patients associates with enhanced antibody efficacy. Together, this work provides preclinical justification and clinical evidence that require prospective investigation of antibody drugs combined with statins to delay drug resistance in tumors.

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