JASPER THERAPEUTICS, INC. Jasper Therapeutics
Corporate Presentation
December 2023
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Forward-Looking Statements
This investor presentation and any accompanying oral presentation (together, this "Presentation") contain forward-looking statements. All statements other than statements of historical fact contained in this Presentation, including statements regarding the future opportunities and prospects of Jasper Therapeutics, Inc. (together with its subsidiary, "Jasper" or the "Company"), including milestones, potential regulatory filings and the anticipated timing thereof, patient enrollment, future timelines, business strategy, and plans and objectives for future operations, are forward-looking statements. Jasper has based these forward-looking statements on its estimates and assumptions and its current expectations and projections about future events. These forward- looking statements are subject to a number of risks, uncertainties and assumptions, including those contained in the "Risk Factors" section of the Company's Annual Report on Form 10-K for the year ended December 31, 2022, Quarterly Reports on Form 10-Q and Current Reports on Form 8-K that the Company has subsequently filed or may subsequently file with the SEC. In light of these risks, uncertainties and assumptions, the forward-looking events and circumstances discussed in this Presentation are inherently uncertain and may not occur, and actual results could differ materially and adversely from those anticipated or implied in the forward-looking statements. Accordingly, you should not rely upon forward-looking statements as predictions of future events. Jasper undertakes no obligation to update publicly or revise any forward-looking statements for any reason after the date of this Presentation or to conform these statements to actual results or to changes in Jasper's expectations.
Industry and Market Data
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Trademarks
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Briquilimab is an investigative | |
drug and is not approved | |
for any indication | 2 |
Briquilimab: Franchise Potential in Mast Cell Diseases
c- | Kit inhibition | • Mast cells are key drivers in immunological and dermatological diseases with high unmet need | ||
• | Mast cell depletion has distinct potential to deliver safe and durable disease control | |||
a | promising new | |||
MOA in mast cell | • | c-Kit inhibition is the only therapeutic mechanism shown to significantly deplete mast cells | ||
diseases | • | c-Kit inhibition has demonstrated clinical proof of concept in multiple mast mediated diseases | ||
Briquilimab | • Briquilimab is a potent c-Kit inhibitor proven to drive mast cell depletion | |||
• | Potency of briquilimab binding could allow for less frequent dosing | |||
a | potent c-Kit | |||
• | Dosing and PK profile could minimize unwanted adverse effects | |||
inhibitor | ||||
• Therapeutic potential extends beyond mast cell diseases into stem cell diseases | ||||
Robust pipeline | • | CSU: First patient dosed in Phase 1b/2a BEACON study (initial data expected mid-year 2024) | ||
multiple company- | • | CIndU - Phase 1b/2a study in the EU initiating early 2024 (initial data expected 2H 2024) | ||
led clinical | ||||
• | LR-MDS - Phase 1 trial in the US ongoing (initial data expected 1H 2024) | |||
programs | ||||
NON-CONFIDENTIAL
Briquilimab is an investigative | |
drug and is not approved | |
for any indication | 3 |
Expanded portfolio presents exciting new opportunities in mast cell diseases
Indication | Sponsor | Research | Preclinical | Clinical | Program Milestones | ||
Briquilimab | |||||||
Mast Cell Diseases (Subcutaneous) | |||||||
• | IND cleared; EU CTA submitted | ||||||
Chronic Spontaneous Urticaria | • | Enrolling | |||||
• | Initial clinical data expected in mid-2024 | ||||||
• | EU CTA submitted | ||||||
Chronic Inducible Urticaria | • | FPI expected in Q1 2024 | |||||
• | Initial clinical data expected in mid-2024 | ||||||
Stem Cell Diseases (Intravenous) | |||||||
Low-to-Intermediate Risk MDS | • | Enrolling | |||||
• | Initial clinical data expected late early 2024 | ||||||
SCID | • | Enrolling | |||||
• | Potential BLA filing | ||||||
Fanconi Anemia | • | First 4 patients achieved full chimerism & count recovery | |||||
• | Expansion to Phase 2a (enrolling) | ||||||
Sickle Cell Disease | • | First 3 patients with full chimerism & Hb increase (enrolling) | |||||
Chronic Granulomatous Disease | • | Enrolling | |||||
GATA2 MDS | • | Study start up | |||||
Investigator Sponsored Studies |
Jasper maintains full worldwide rights to develop and commercialize briquilimab in all indications
Briquilimab is an investigative | |
drug and is not approved | |
for any indication | 4 |
SCF blockade drives differential impact on mast cells and stem cells
Briquilimab | Stem Cell Factor (SCF) | Briquilimab | Stem Cell Factor (SCF) |
MAST CELLS (MC)
ckit
MC | ||
P13K | Apoptosis | |
MC | MC | |
AKT | BIM |
FOXO3A
MC
MC Apoptosis
APOPTOTIC MC
Programmed Cell Death
ckit
CYCLING HSC | |||
Quiescent HSC | |||
FLT3 | SCF Signaling | Quiescent HSC | |
Growth | Self-Renewal | ||
TPO | Factor | ||
Signaling | |||
MPL |
Differentiation
Quiescent HSC
HSC Differentiation
MEGAKARYOCYTE
Quiescent HSC
STEM CELLS (HSC)
Apoptotic MC
Apoptotic MC
Quiescent HSC
Durable
Depletion
Apoptotic MC
Quiescent HSC | Exit BM |
Niche | |
Briquilimab is an investigative drug and is not approved
for any indication | 5 |
Mast cells are key drivers of the inflammatory response in a number of allergic and dermatologic diseases
- Mast cells are the most potent drivers of inflammatory response in skin, lungs and gut
- Activated mast cells release pro-inflammatory compounds that drive diseases such as Chronic Spontaneous Urticaria, Chronic Inducible Urticaria, Asthma and many others
- Current approved therapies targeting mast cell driven diseases have limited efficacy and limited durability of response
Briquilimab is an investigative | ||
drug and is not approved | ||
Theoharides et al. N Engl J Med. (2015) | for any indication | 6 |
Depletion of mast cells by anti-c-Kit monoclonal antibody blockade is a novel approach to treat urticarias and other mast cell mediated diseases
- SCF signaling through c-Kit prevents mast cells apoptosis via the Bim-mediated pathway1
- Blockade of c-Kit signaling on mast cells leads to organized cell death and phagocytic clearance2
- Partial c-Kit inhibition blunts mast cell activation
- Aglycosylated c-Kit antibodies avoid indiscriminate ADCC driven killing of other c-Kit expressing cells3
- Unwanted effects on other c-Kit expressing cells can be minimized by the recovery of c-Kit signaling once the mast cells are depleted
- Moller C et al. Blood (2005)
- Hundley TR et al. Blood (2004)
- Arnold JN et al. Annu Rev Immunol (2007)
Briquilimab-Mediated
Mast Cell Apoptosis
Briquilimab is an investigative | |
drug and is not approved | |
for any indication | 7 |
Briquilimab potently blocks c-Kit signaling leading to durable mast cell depletion
Mast cell survival assay1
- Briquilimab is an aglycosylated IgG1 anti c-Kit antibody with high affinity to c-Kit (Kd <5pm)
- Briquilimab potently blocks c-Kit signaling by blocking the SCF ligand binding site on the receptor and triggering apoptosis
- Mast cell depletion occurs within hours to days
Briquilimab is an investigative | ||
drug and is not approved | ||
1 Jasper internal data | for any indication | 8 |
Briquilimab delivered with a single subcutaneous injection significantly depletes mast cells in humans above 0.8 mg/kg threshold
- A single subcutaneous dose above ~0.8 mg/kg potently depletes mast cells in the skin of healthy volunteers
- Skin mast cell depletion highly correlated to serum briquilimab exposure after subcutaneous administration
- Significant depletion by day 7, with durable response lasting at least 29 days
- Once depleted with an anti-c-Kit antibody, skin mast cells take at least 3 months to recover, potentially leading to durable disease control2
Skin mast cell depletion 4 weeks after single dose (≥42 mg)1
Briquilimab Healthy Volunteer Phase 1 Subcutaneous Study
0.8 mg/kg
1 | Jasper internal data (Phase 1a, healthy volunteer study); Dose is adjusted to body weight (mg/kg) on graph. Skin biopsies were used to count mast cells. | Briquilimab is an investigative | |
drug and is not approved | |||
2 | Maurer et al, GA²LEN Global Urticaria Forum - Berlin, December 6, 2022 | for any indication | 9 |
Briquilimab's favorable pharmacokinetic properties may enable optimal biologic dosing
- Briquilimab is designed to minimize unwanted c-Kit-related effects
- Subcutaneous dosing leads to predictable PK profile
- Low frequency of ADAs and do not appear to affect PK
- Drug elimination profile is favorable for minimizing off target effects
- Clearance to allow for return of c-Kit signaling once the mast cells are depleted
- No modifications to extend FcRn recycling
Pharmacokinetics (≥10 mg)1
Briquilimab Healthy Volunteer Phase 1 Subcutaneous Study
Briquilimab is an investigative | ||
drug and is not approved | ||
1 Jasper internal data (Phase 1a, healthy volunteer study) | for any indication | 10 |
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Jasper Therapeutics Inc. published this content on 21 December 2023 and is solely responsible for the information contained therein. Distributed by Public, unedited and unaltered, on 25 December 2023 00:39:37 UTC.
