Monitoring Melanoma Responses to STING Agonism and Focused Ultrasound Thermal Ablation Using Microneedles and Ultrasensitive Single Molecule Arrays

Author:

Dahis Daniel1234ORCID,Dion Michelle Z.2345,Cryer Alexander M.234,Dosta Pere234ORCID,Gilboa Tal46,Alonso Mariana3,Lewandowski Michael4,Puigmal Núria234,Taboada Gonzalo Muñoz2ORCID,Azhari Haim1ORCID,Ahmad Rushdy4,Walt David R.46ORCID,Artzi Natalie2347ORCID

Affiliation:

1. Technion Institute of Technology Haifa 320003 Israel

2. Institute for Medical Engineering and Science Massachusetts Institute of Technology Cambridge MA 02139 USA

3. Brigham and Women's Hospital Harvard Medical School Boston MA 02115 USA

4. Wyss Institute for Biologically‐Inspired Engineering Harvard University Boston MA 02115 USA

5. Harvard‐MIT Division of Health Sciences & Technology, Massachusetts Institute of Technology, Cambridge, MA, USA Cambridge 02139 United States

6. Department of Pathology, Brigham and Women's Hospital Harvard Medical School Boston Boston MA 02115 USA

7. Broad Institute of Harvard and MIT Cambridge MA 02139 USA

Abstract

AbstractReal‐time monitoring of immune state and response to therapy can provide a means to stratify patients and increase the number of responders who will benefit from approved and emerging immunotherapies. The accessibility of immune cells in the skin provides an opportunity for local immune modulation as well as for noninvasive sampling of disease biomarkers in the skin interstitial fluid (ISF). Here, a monitoring strategy for melanoma immunotherapy is investigated by longitudinal sampling of biomarkers in the skin ISF using Hyaluronic acid (HA)‐based microneedles (MNs). Focused ultrasound ablation and delivery of nanoparticulate stimulator of interferon genes agonist are used as model immunotherapies. It is shown that this combination therapy induces potent inflammatory responses in a melanoma mouse model, promoting tumor elimination and immune memory formation. Indeed, quantifying soluble, protein‐based biomarkers following therapy using conventional immunoassay reveals a pronounced proinflammatory program in the tumor. However, conventional assays fail to detect the low concentration of biomarkers in plasma and in MN‐sampled ISF. It is shown that ultrasensitive single molecule arrays (Simoa) effectively detected proinflammatory biomarkers that are upregulated in response to the therapy in MN‐sampled ISF, in plasma, and in tumors, supporting the feasibility of monitoring melanoma immunotherapy using MNs.

Funder

European Association for Cancer Research

United States - Israel Binational Science Foundation

Publisher

Wiley

Subject

Electrochemistry,Condensed Matter Physics,Biomaterials,Electronic, Optical and Magnetic Materials

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