Just going to drop this here - rather than clog up the other threads.
https://newatlas.com/medical/cancer-immunotherapy-stem-cell-rejuvenation/
Its an interesting article, based on early stage research out of japan ( published in the journal of molecular therapy) about "supercharging Car-T" cells by turning them back to Pluripotent stem cells before growing and multiplying them. - This also allows the insertion of other molecular targets, making the CAR-T immunooncology product more robust, wider targeted, AND longer lasting.
Specifically of interest to me was some side research they mentioned on CD-19. Which of course is our target protein of choice for CF33.
i am no expert in microbiology - however I am an educated layperson, my interpretation ( and i am * completely open* to being corrected) LOL, is that making any potential big pharma partner's CD19 targeting Car-T therapies, more potent and longer lasting, is a perfect value add to our CF33 product.
We will paint the CD-19 target on solid tumors, give the tumor a stiff uppercut with CF33 and our partners can hit it with a supercharged, customised longlasting "CD19 seeking" Car-T response.
Obviously this is still in murine tests and is a long way from a commercial approach or product - however I like doing research, and *anything* that works or enhances CD-19 Car-T therapies, is of particular interest.
I like the fact that Paul Hoppers company ( IMU CHAIRPERSON) "Chimeric theraputics" ( ASX:CHM) is currently working on CAR-T therapies with payloads derived from scorpion venom. so I suppose im just interested in potential collaberations and co-operations down the road...
anyway - its just a thought bubble - however the research shows that there are signicant discoveries and finetuning going on in the big bad world of Car-T therapies and immunoncology. which only augurs well for our flagship product
APO!
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