Deficiency of host CD96 and PD-1 or TIGIT enhances tumor immunity without significantly compromising immune homeostasis
Multiple non-redundant immunosuppressive pathways co-exist in the tumor microenvironment and their co-targeting can increase clinical responses. Indeed, concurrent blockade of CTLA-4 and PD-1 in patients with advanced melanoma increased clinical responses over monotherapy alone although the frequenc...
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Veröffentlicht in: | Oncoimmunology 2018-07, Vol.7 (7), p.e1445949-e1445949 |
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Sprache: | eng |
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Zusammenfassung: | Multiple non-redundant immunosuppressive pathways co-exist in the tumor microenvironment and their co-targeting can increase clinical responses. Indeed, concurrent blockade of CTLA-4 and PD-1 in patients with advanced melanoma increased clinical responses over monotherapy alone although the frequency and severity of immune related adverse events (irAEs) also increased. Nevertheless, a substantial number of patients still display an innate resistance phenotype and are unresponsive to current approved immunotherapies even when utilized in combination. In this study, we generated Pdcd1
−
/
−
CD96
−
/
−
and Tigit
−
/
−
CD96
−
/−
mice to investigate how loss of CD96 in combination with PD-1 or TIGIT impacts on immune homeostasis and hence the potential of inducing immune related toxicities following co-targeting of these pairs of receptors. The ability of Pdcd1
−
/
−
CD96
−
/
−
and Tigit
−
/
−
CD96
−
/−
mice to suppress primary tumor growth was also assessed using the MC38 colon carcinoma and SM1WT1 BRAF-mutated melanoma tumor models. Both Pdcd1
−
/
−
CD96
−
/
−
or Tigit
−
/
−
CD96
−
/−
mice displayed no overt perturbations in immune homeostasis over what was previously reported with Pdcd1
−
/
−
or Tigit
−
/
−
mice even when aged for 22 months. Interestingly, increased suppression of subcutaneous tumor growth and complete responses was seen in Pdcd1
−
/
−
CD96
−
/
−
mice compared to Pdcd1
−
/
−
or CD96
−
/
−
mice depending upon the tumor model. In contrast, in these models, growth suppression in Tigit
−
/
−
CD96
−
/
−
were similar to Tigit
−
/
−
or CD96
−
/
−
. This enhanced anti-tumor efficacy of Pdcd1
−
/
−
CD96
−
/
−
appeared to be due to favorable changes in the ratio of CD8
+
T cells to T regulatory cells or CD11b
+
GR-1
hi
myeloid cells in the tumor microenvironment. Co-targeting CD96 and PD-1 may increase anti-tumor immunity over targeting PD-1 alone and potentially not induce serious immune-related toxicities and thus appears a promising strategy for clinical development. |
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ISSN: | 2162-4011 2162-402X 2162-402X |
DOI: | 10.1080/2162402X.2018.1445949 |