Kymera’s novel MDM2 degrader granted orphan designation for AML

Phase 1Orphan DrugFast TrackClinical Result
Kymera’s novel MDM2 degrader granted orphan designation for AML
Preview
Source: Pharmaceutical Technology
Aidan McNamee
Kymera’s novel MDM2 degrader granted orphan designation for AML
Preview
Source: Pharmaceutical Technology
Kymera’s KT-253 is being explored in a variety of liquid and solid tumours. Source: Shutterstock / Juan Gaertner.
Clinical-stage biopharma Kymera Therapeutics has announced that the US Food and Drug Administration (FDA) has granted KT-253 orphan drug designation for treating acute myeloid leukaemia (AML).
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Kymera’s novel MDM2 degrader granted orphan designation for AML
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KT-253 is a highly potent and selective degrader. It targets MDM2, the regulator of common tumour suppressor p53. The p53 protein remains intact in nearly half of all cancers, retaining the ability to limit cancer cell growth, Existing inhibitors manage to improve p53 expression, but in turn, also increase MDM2 and limit its efficacy.
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A phase I study (NCT05775406) of KT-253, initiated in March 2023, is currently ongoing. It is evaluating the safety, tolerability, pharmacokinetics, and pharmacodynamics of KT-253 in patients with relapsed or refractory high-grade myeloid malignancies, including AML, acute lymphocytic leukaemia (ALL), lymphoma and solid tumours.
Kymera claims that KT-253 is able to avoid an increase in MDM2 and kill cancer cells, even with brief exposures. As a result, it is being explored for AML, as well as a variety of other liquid and solid tumours.
Kymera Therapeutics founder, president and CEO Nello Mainolfi welcomed the designation, hailing it as “a significant opportunity to deliver an important new medicine” that can target a protein that conventional medicines had often struggled with.
This marks yet another protein degrader developed with the company’s proprietary drug discovery platform, Pegasus. Kymera claims that Pegasus can harness the body’s innate protein recycling machinery to degrade dysregulated, disease-causing proteins. Currently, the company is pursuing programmes to target IRAK4, IRAKIMiD, and STAT3 within the IL-1R/TLR or JAK/STAT pathways. It hopes to produce treatments for a variety of immune-inflammatory diseases, hematologic malignancies, and solid tumours.
Previously, Sanofi paid $150m for a multi-programme collaboration with Kymera. The agreement, eligible for additional payments of up to $2bn, is intended to develop and commercialise IRAK4 protein degraders like KT-474. Results from a Phase I trial (NCT04772885) published in May 2023 showed promise for KT-474 in treating hidradenitis suppurativa and atopic dermatitis. A Phase II trial is expected to commence later this year.
Kymera also partnered with Vertex Therapeutics in a $70m deal. The two companies will work together to develop various protein degradation medicines, with Vertex having an option to exclusively license discovered molecules.
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How is the Biopharmaceutical industry evolving?
2021 was a year of continued innovation and change in the Biopharmaceutical industry. As the COVID-19 pandemic continues to take its toll on businesses worldwide, it’s time to look for new ways to create value, prepare for the future, and remain competitive in the ever-changing landscape.
GlobalData’s expansive report examines the business environment and trends that shape the Biopharmaceutical industry. We highlight the most impactful emerging technologies, as well as the industry, regulatory, and macroeconomic factors that influence growth prospects.
Access the report to:
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Gain a deeper "on the ground" perspective through exclusive opinions and analysis from industry respondents.
Evaluate the effects of COVID-19 on the sector.
Download the full report to understand what to expect and how to align your strategies for success.
By GlobalData
Kymera’s novel MDM2 degrader granted orphan designation for AML
Preview
Source: Pharmaceutical Technology
Submit
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Mali (+223)
Malta (+356)
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Mayotte (+269)
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Mongolia (+976)
Montserrat (+1664)
Morocco (+212)
Mozambique (+258)
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Namibia (+264)
Nauru (+674)
Nepal (+977)
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New Caledonia (+687)
New Zealand (+64)
Nicaragua (+505)
Niger (+227)
Nigeria (+234)
Niue (+683)
Norfolk Islands (+672)
Northern Marianas (+670)
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Papua New Guinea (+675)
Paraguay (+595)
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Suriname (+597)
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Syria (+963)
Taiwan (+886)
Tajikstan (+7)
Thailand (+66)
Togo (+228)
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Tunisia (+216)
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Turkmenistan (+993)
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Réunion
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Saint Helena, Ascension and Tristan da Cunha
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