EMBO Molecular Medicine (Jun 2019)

Functional systemic CD4 immunity is required for clinical responses to PD‐L1/PD‐1 blockade therapy

  • Miren Zuazo,
  • Hugo Arasanz,
  • Gonzalo Fernández‐Hinojal,
  • Maria Jesus García‐Granda,
  • María Gato,
  • Ana Bocanegra,
  • Maite Martínez,
  • Berta Hernández,
  • Lucía Teijeira,
  • Idoia Morilla,
  • Maria Jose Lecumberri,
  • Angela Fernández de Lascoiti,
  • Ruth Vera,
  • Grazyna Kochan,
  • David Escors

DOI
https://doi.org/10.15252/emmm.201910293
Journal volume & issue
Vol. 11, no. 7
pp. 1 – 14

Abstract

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Abstract The majority of lung cancer patients progressing from conventional therapies are refractory to PD‐L1/PD‐1 blockade monotherapy. Here, we show that baseline systemic CD4 immunity is a differential factor for clinical responses. Patients with functional systemic CD4 T cells included all objective responders and could be identified before the start of therapy by having a high proportion of memory CD4 T cells. In these patients, CD4 T cells possessed significant proliferative capacities, low co‐expression of PD‐1/LAG‐3 and were responsive to PD‐1 blockade ex vivo and in vivo. In contrast, patients with dysfunctional systemic CD4 immunity did not respond even though they had lung cancer‐specific T cells. Although proficient in cytokine production, CD4 T cells in these patients proliferated very poorly, strongly co‐upregulated PD‐1/LAG‐3, and were largely refractory to PD‐1 monoblockade. CD8 immunity only recovered in patients with functional CD4 immunity. T‐cell proliferative dysfunctionality could be reverted by PD‐1/LAG‐3 co‐blockade. Patients with functional CD4 immunity and PD‐L1 tumor positivity exhibited response rates of 70%, highlighting the contribution of CD4 immunity for efficacious PD‐L1/PD‐1 blockade therapy.

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