Cancers (Feb 2022)

Imaging Kv1.3 Expressing Memory T Cells as a Marker of Immunotherapy Response

  • Julian L. Goggi,
  • Shivashankar Khanapur,
  • Boominathan Ramasamy,
  • Siddesh V. Hartimath,
  • Tang Jun Rong,
  • Peter Cheng,
  • Yun Xuan Tan,
  • Xin Yi Yeo,
  • Sangyong Jung,
  • Stephanie Shee Min Goay,
  • Seow Theng Ong,
  • You Yi Hwang,
  • K. George Chandy,
  • Edward G. Robins

DOI
https://doi.org/10.3390/cancers14051217
Journal volume & issue
Vol. 14, no. 5
p. 1217

Abstract

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Immune checkpoint inhibitors have shown great promise, emerging as a new pillar of treatment for cancer; however, only a relatively small proportion of recipients show a durable response to treatment. Strategies that reliably differentiate durably-responding tumours from non-responsive tumours are a critical unmet need. Persistent and durable immunological responses are associated with the generation of memory T cells. Effector memory T cells associated with tumour response to immune therapies are characterized by substantial upregulation of the potassium channel Kv1.3 after repeated antigen stimulation. We have developed a new Kv1.3 targeting radiopharmaceutical, [18F]AlF-NOTA-KCNA3P, and evaluated whether it can reliably differentiate tumours successfully responding to immune checkpoint inhibitor (ICI) therapy targeting PD-1 alone or combined with CLTA4. In a syngeneic colon cancer model, we compared tumour retention of [18F]AlF-NOTA-KCNA3P with changes in the tumour immune microenvironment determined by flow cytometry. Imaging with [18F]AlF-NOTA-KCNA3P reliably differentiated tumours responding to ICI therapy from non-responding tumours and was associated with substantial tumour infiltration of T cells, especially Kv1.3-expressing CD8+ effector memory T cells.

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