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31.01.2020 | Research Article

Examining Immunotherapy Response Using Multiple Radiotracers

verfasst von: Julian L Goggi, Siddesh V Hartimath, Youyi Hwang, Yun Xuan Tan, Shivashankar Khanapur, Boominathan Ramasamy, Lingfan Jiang, Fui Fong Yong, Peter Cheng, Peng Wen Tan, Mohamed AR Husaini, Tsz Ying Yuen, Beverly Jieu, Ann-Marie Chacko, Anis Larbi, Laurent Renia, Charles Johannes, Edward G Robins

Erschienen in: Molecular Imaging and Biology | Ausgabe 4/2020

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Abstract

Purpose

Cancer immunotherapy has shown huge potential in the fight against cancer, but only a small proportion of patients respond successfully to treatment. Non-invasive methods to stratify responders from non-responders are critically important as immune therapies are often associated with immune-related side effects. Currently, conventional clinical imaging modalities do not provide a useful measure of immune therapy efficacy. Sensitive imaging biomarkers that provide information about the tumoural microenvironment may provide useful insights allowing for improved patient management.

Procedures

We have assessed the ability of a number of radiopharmaceuticals to non-invasively measure different aspects of the tumour microenvironment and correlated tumour uptake to immune therapy response in a syngeneic model of colon cancer, CT26-WT. Four radiopharmaceuticals, [¹⁸F]FDG (a glucose analogue), [¹⁸F]FEPPA (a marker for macrophage activation), [¹⁸F]FB-IL2 (a marker for CD25⁺ cells) and [⁶⁸Ga] Ga-mNOTA-GZP (a marker for granzyme B, the serine protease downstream effector of cytotoxic T cells), were assessed as potential biomarkers to help stratify response to PD-1 monotherapy or combined anti-PD1 and CLTA4 therapy in vivo correlating tumour uptake with changes in tumour-associated immune cell populations.

Results

[¹⁸F]FDG, [¹⁸F]FEPPA and [¹⁸F]FB-IL2 (a marker for CD25⁺ cells) showed limited ability to determine therapy response and showed little correlation to tumour-associated immune cell changes. However, [⁶⁸Ga] Ga-mNOTA-GZP showed good predictive ability and correlated well with changes in tumour-associated T cells, especially CD8⁺ T cells.

Conclusions

[⁶⁸Ga]Ga-mNOTA-GZP uptake correlates well with changes in CD8⁺ T cell populations supporting continued development of granzyme B-based imaging agents for stratification of response to immunotherapy. Early assessment of immunotherapy efficacy with [⁶⁸Ga]Ga-mNOTA-GZP may allow for the reduction of unnecessary side effects while significantly improving patient management.

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Titel: Examining Immunotherapy Response Using Multiple Radiotracers
verfasst von: Julian L Goggi
Siddesh V Hartimath
Youyi Hwang
Yun Xuan Tan
Shivashankar Khanapur
Boominathan Ramasamy
Lingfan Jiang
Fui Fong Yong
Peter Cheng
Peng Wen Tan
Mohamed AR Husaini
Tsz Ying Yuen
Beverly Jieu
Ann-Marie Chacko
Anis Larbi
Laurent Renia
Charles Johannes
Edward G Robins
Publikationsdatum: 31.01.2020
Verlag: Springer International Publishing
Erschienen in: Molecular Imaging and Biology / Ausgabe 4/2020
Print ISSN: 1536-1632
Elektronische ISSN: 1860-2002
DOI: https://doi.org/10.1007/s11307-020-01477-w

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Examining Immunotherapy Response Using Multiple Radiotracers