The Immune System
Had A Blueprint All Along.

We finally built from it.

CAR-T was invented before scientists fully understood how T cell receptors work. That single architectural gap created many of the limitations the field still faces today: toxic side effects, lack of persistence, cell exhaustion, relapse, and no path beyond heme malignancies.

The Problem

Cell therapies changed oncology.
They just can’t reach everyone who needs it.

Why First-Gen Cell Therapy Falls Short

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Toxic
Side Effects

Uncontrolled immune activation limits who can safely receive treatment.

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Preconditioning Needed

The need for the use of toxic chemotherapies and preconditioning regimens often exacerbate the patient state and add on to the toxic side effects.

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Cell
Exhaustion & Relapse

Cells burn out. Patients who achieved
remission lose it.

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Solid Tumors Unreachable

The majority of cancer diagnoses remain beyond
first-gen therapy.

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Manufacturing Bottleneck

Weeks of production. Extraordinary cost. Many patients
can't wait.

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Cost

The price point for autologous CAR-Ts, TILs, and TCR technology is untenable and unsustainable for the majority of patients worldwide.

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Disease
Restriction

Limited ability to translate to chronic diseases, such as autoimmune, inflammation, and CNS.

Our Solution

The blueprint was always there.
It took 30 years of science to act on it.

Next-generation immune receptor with separate targeting and signaling. On/off control. Bispecific options. No exhaustion. Validated across five cell types.

The Modulari-T SCIENCE

Two technologies. One system. Built from scratch.

MARC-Modular Actuation Receptor Complex

Next-generation immune receptor with separate targeting and signaling. 
On/off control. No exhaustion. Validated across five cell types.

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MoVe-Modular Vector

First rationally designed delivery vehicle for in vivo cell and gene therapy. No liver toxicity. Precisely target immune or non-immune cells.

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