2018
DOI: 10.1158/1538-7445.am2018-2776
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Abstract 2776: MEDI5752: A novel bispecific antibody that preferentially targets CTLA-4 on PD-1 expressing T-cells

Abstract: Studies have demonstrated that the clinical benefit of PD-1 blockade can be further improved by combination with an αCTLA-4 mAb in some indications. However, this increased activity is commensurate with significant immune related adverse events (irAE's). Therefore, novel approaches are required to uncouple toxicity from anti-tumour efficacy and realise the full potential of this combination. MEDI5752 is a monovalent bispecific human IgG1 monoclonal antibody (mAb) with an engineered fragment crystallisable (Fc)… Show more

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Cited by 15 publications
(9 citation statements)
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“…For instance, PD-1/PD-L1 axis inhibition was shown to improve anti-tumour efficacy by reversing related immune resistance when used in combination with various types of T cell engagers, including αHER2 × αCD3, 162 αCEA × αCD3, 163 αCD33 × αCD3, 164 αTrop-2 × αCD3 and αCEACAM5 × αCD3 BsAbs. 165 Numerous other examples of immunomodulatory antibodies used in combination therapy, not only with BsAbs, have been reported and reviewed, notably by Patel et al 166 Two immunomodulators can also be combined into the same BsAb, generating a dual immunomodulatory BsAb that has the potential to: (1) avoid immune escape by blocking two different inhibitory immune checkpoints (such dual immune checkpoint inhibitory BsAbs include αPD-1 × αCTLA-4, αPD-1 × αTIM-3, and αPD-1 × αLAG3 bispecifics 167–169 ); (2) induce a strong stimulation and expansion of T cells when combining two immunostimulators ( e.g. dual agonistic BsAb αCD137 × αOX40); 170 and (3) induce a synergistic effect when blocking an inhibitory immune checkpoint and activating a stimulatory immune checkpoint – this type of BsAb is sometimes defined as an agonist redirected checkpoint (αPD-1 × αOX40, αCTLA-4 × αOX40).…”
Section: Bispecific Antibodies In Immunotherapymentioning
confidence: 99%
“…For instance, PD-1/PD-L1 axis inhibition was shown to improve anti-tumour efficacy by reversing related immune resistance when used in combination with various types of T cell engagers, including αHER2 × αCD3, 162 αCEA × αCD3, 163 αCD33 × αCD3, 164 αTrop-2 × αCD3 and αCEACAM5 × αCD3 BsAbs. 165 Numerous other examples of immunomodulatory antibodies used in combination therapy, not only with BsAbs, have been reported and reviewed, notably by Patel et al 166 Two immunomodulators can also be combined into the same BsAb, generating a dual immunomodulatory BsAb that has the potential to: (1) avoid immune escape by blocking two different inhibitory immune checkpoints (such dual immune checkpoint inhibitory BsAbs include αPD-1 × αCTLA-4, αPD-1 × αTIM-3, and αPD-1 × αLAG3 bispecifics 167–169 ); (2) induce a strong stimulation and expansion of T cells when combining two immunostimulators ( e.g. dual agonistic BsAb αCD137 × αOX40); 170 and (3) induce a synergistic effect when blocking an inhibitory immune checkpoint and activating a stimulatory immune checkpoint – this type of BsAb is sometimes defined as an agonist redirected checkpoint (αPD-1 × αOX40, αCTLA-4 × αOX40).…”
Section: Bispecific Antibodies In Immunotherapymentioning
confidence: 99%
“…MEDI5752 (PD-1×CTLA-4) inhibits the function of CTLA-4 in PD-1 + activated T cells, inducing rapid internalization and degradation of PD-1. Also, MEDI5752 showed enhanced activity compared to that of the combination of PD-1 and CTLA-4 mAb treatment ( 41 42 ). Functional inhibitors targeting other checkpoint molecules, including LAG-3 and TIM-3, are under development ( 43 44 ).…”
Section: Functional Mechanisms Of Bsabmentioning
confidence: 99%
“…For example, MEDI5752 (PD-1 × CTLA-4) is a monovalent BsAb that inhibits PD-1 and CTLA-4 with reduced Fc function and was designed to block CTLA-4-mediated inhibition on PD-1 + T cells. Upon binding to targets, MEDI5752 is rapidly internalized and leads to the subsequent degradation of PD-1, which is not observed with mAbs [ 113 , 114 ]. BsAbs targeting LAG-3, Tim-3, and TIGIT with PD-(L)1 have been developed actively because of better efficacy than combinations in preclinical studies [ 115 ].…”
Section: Dual Immunomodulatorsmentioning
confidence: 99%