24.04.2025

Researchers at Helmholtz Munich and the Technical University of Munich have created a next-generation delivery system that significantly improves the transport of gene-editing tools into living cells. The system, named ENVLPE, uses non-infectious, virus-like particles to efficiently deliver molecular editors like CRISPR/Cas9 into target cells.

Image: A virus-like particle floats above a cell with double-stranded DNA protruding from it; Copyright: Dong-Jiunn Jeffery Truong

The ENVLPE system uses virus-like particles to safely introduce molecular gene editors such as CRISPR into target cells to make targeted DNA corrections.

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Key features of ENVLPE include:

Use of engineered, non-infectious viral shells as delivery vehicles

Packaging of fully assembled gene editors

A protective molecular shield for vulnerable components

Compatibility with base editors and prime editors

Efficient intracellular assembly through redirected transport pathways

Restoring vision in mouse models of genetic blindness

In a collaborative study with UC Irvine, the ENVLPE system was tested in a mouse model with inherited blindness caused by a mutation in the Rpe65 gene.

“The mice carry a disabling mutation in the Rpe65 gene, which is essential for producing light-sensitive molecules in the retina, and therefore are fully blind and unresponsive to light,” explains Samuel W. Du. After injection of ENVLPE into the subretinal space, the animals began responding to light stimuli. “The extent of restoration was astounding,” adds Julian Geilenkeuser.

Compared to other systems, ENVLPE required more than ten times less dosage to achieve similar results. “We resolved critical bottlenecks and achieved a much more efficient packaging by the delivery agents,” says Niklas Armbrust.

Expanding potential: universal T cells for cancer therapy

Beyond gene therapy for genetic disorders, ENVLPE also enables genetic modification of T cells for cancer immunotherapy. In cooperation with TUM University Hospital, ENVLPE was used to remove specific surface proteins from T cells to prevent immune rejection. This paves the way for universal T cells that are not restricted to individual patients.

These advances support both:

In vivo gene therapies for inherited diseases

Ex vivo cell therapies for cancer

Prof. Gil Westmeyer emphasizes: “The highly modular ENVLPE system brings us substantially closer to on-demand and precise genetic modifications of complex cellular models.”

MEDICA-tradefair.com; Source: Helmholtz Munich

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