Abstract 2861: TriTAC-XR: An extended-release T cell engager platform designed to minimize cytokine release syndrome

Kwant, Kathryn; Rocha, Sony S.; Yu, Timothy; Stephenson, Katrina; Banzon, Raphaela Rose; Vollhardt, Sydney; Hemmati, Golzar; Callihan, Evan; Aaron, Wade; Thothathri, Subramanian; O'Rear, Jessica; Bragg, Eric; Kwong, Willis; Situ, Hubert; Hundal, Avneel; Yu, Stephen; Jackson, Taggra; Carlin, Kevin; Xiao, Yinghua; Dayao, Maria Rosalyn; To, Linh; Bergo, Nick; Wright, Kevin J.; Austin, Robert J.; Wesche, Holger; Lemon, Bryan; Lin, Sen

doi:10.1158/1538-7445.am2022-2861

Cited by 1 publication

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“…Of note, other conditionally active TCE are designed for prolonged release, which could benefit a wider range of patients. One example is the TriTAC-XR, an extended-release TCE platform designed to minimize CRS by reducing maximum drug concentration in systemic circulation [140].…”

Section: Prevention Of Treatment-related Adverse Eventsmentioning

confidence: 99%

Bi- and trispecific immune cell engagers for immunotherapy of hematological malignancies

Tapia-Galisteo,

Álvarez-Vallina,

Sanz

2023

J Hematol Oncol

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Immune cell engagers are engineered antibodies with at least one arm binding a tumor-associated antigen and at least another one directed against an activating receptor in immune effector cells: CD3 for recruitment of T cells and CD16a for NK cells. The first T cell engager (the anti-CD19 blinatumomab) was approved by the FDA in 2014, but no other one hit the market until 2022. Now the field is gaining momentum, with three approvals in 2022 and 2023 (as of May): the anti-CD20 × anti-CD3 mosunetuzumab and epcoritamab and the anti-B cell maturation antigen (BCMA) × anti-CD3 teclistamab, and another three molecules in regulatory review. T cell engagers will likely revolutionize the treatment of hematological malignancies in the short term, as they are considerably more potent than conventional monoclonal antibodies recognizing the same tumor antigens. The field is thriving, with a plethora of different formats and targets, and around 100 bispecific T cell engagers more are already in clinical trials. Bispecific NK cell engagers are also in early-stage clinical studies and may offer similar efficacy with milder side effects. Trispecific antibodies (engaging either T cell or NK cell receptors) raise the game even further with a third binding moiety, which allows either the targeting of an additional tumor-associated antigen to increase specificity and avoid immune escape or the targeting of additional costimulatory receptors on the immune cell to improve its effector functions. Altogether, these engineered molecules may change the paradigm of treatment for relapsed or refractory hematological malignancies.

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Section: Prevention Of Treatment-related Adverse Eventsmentioning

confidence: 99%