Tech at Polsky

Nanomaterial Based Intracellular Drug Delivery Of Therapeutic Peptides

Inventor(s):

Technology Classifications > Therapeutics

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SUMMARY

Intracellular delivery involves introduction of small biomolecules, nucleic acids, proteins, synthetic nanomaterials and drugs into the cell.
There is a lot of focus on targeted intracellular delivery for improved therapy of cancer and intracellular infections. Intracellular delivery of various drugs can sharply increase the efficiency of various treatment protocols.
The inventors have developed polymersome nanoparticles to deliver cargo such as stapled peptides.
The proof of concept particle is a CD19 Fab linked to the polymersome through a cysteine linker and the stapled peptides (SAH-MS1-18) are enveloped by the polymer.

FIGURE

A schematic of CD19-targeted polymersomes deliver SAH-MS1-18 into the cytoplasm of human diffuse large B-cell lymphoma (DLBCL) cells to reactivate cell death and synergize with p53-reactivation. (a) Cancer cells rely on PPIs for inhibition of apoptosis (e.g. MCL-1 sequesters pro-apoptotic proteins). (b) Therapeutic stapled peptides (e.g. SAH-MS1-18) can potently and specifically block a disease-driving PPI. (c) Cellular uptake is a major obstacle to the clinical translation of therapeutic stapled peptides. (d) Stapled peptides are stably encapsulated in PEG-SS-PPS polymersomes. (e) Recombinant αCD19 Fabs are functionalized with a site-specific click chemistry handle. (f) The polymersomes are decorated with αCD19 Fabs and the targeted polymersomes (αCD19-PSOMs) purified. (g) αCD19-PSOMs bind CD19 on DLBCL cells and initiate endocytosis. (h) In the relatively reducing endosome, the disulfide of PEG-SSPPS is reduced. (i) Polymersomes are disrupted and release their cargo. (j) The hydrophobic PPS block facilitates endosomal escape. (k) SAH-MS1-18 binds MCL-1 in the cytoplasm to release pro-apoptotic proteins and (l) reactivate apoptosis if the cell is sufficiently primed to die. (m) Systemic treatment with the p53-reactivating stapled peptide ATSP-7041 (n) inhibits p53's inhibitory binding partners. (o) In cancer cells, phosphorylated/activated p53 translocates to the nucleus to upregulate transcription of pro-apoptotic proteins (e.g. PUMA, 25 BAX) and downregulate transcription of anti-apoptotic proteins (e.g. BCL-2). (p) p53 transcriptional changes sensitize DLBCL to cell death by MCL-1 inhibition.

ADVANTAGES

The approach allows an efficient delivery of biologic therapeutics such as stapled peptides using nanomaterials since peptides typically are not cell permeable.
The lower density of the targeting Fab facilitates better delivery.
The CD19-targeted polymersomes greatly improved the uptake and endosomal escape of therapeutic peptides, amplifying their therapeutic effects by orders of magnitude.

APPLICATIONS

The potential applications lie in more efficient intracellular drug delivery of stapled peptides for treatment of cancer.
This technology improves upon prior PEG-SS-PPS polymersomes by targeting them to specific cell surface receptors for targeted delivery, rather than uptake through non-specific endocytosis/phagocytosis.

PUBLICATIONS

Schnorenberg MR, Hawley KM, Thomas-Toth AT, Watkins EA, Tian Y, Ting JM, Leak LB, Kucera IM, Raczy MM, Kung AL, Hubbell JA, Tirrell MV, LaBelle JL. Targeted Polymersome Delivery of a Stapled Peptide for Drugging the Tumor Protein p53:BCL-2-Family Axis in Diffuse Large B-Cell Lymphoma. ACS Nano. 2023 Dec 12;17(23):23374-23390. doi: 10.1021/acsnano.3c04112. Epub 2023 Sep 9. PMID: 37688780; PMCID: PMC10722602.

TECH DETAILS

Published
1/3/2022

Reference ID
21-T-027