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home / articles / APRE - Aprea Therapeutics Announces Presentations on its Next Generation WEE1 Inhibitor APR-1051 and A Novel Macrocyclic ATR Inhibitor ATRN-119 at AACR Annual Meeting 2024 | Benzinga

APRE - Aprea Therapeutics Announces Presentations on its Next Generation WEE1 Inhibitor APR-1051 and A Novel Macrocyclic ATR Inhibitor ATRN-119 at AACR Annual Meeting 2024 | Benzinga

Aprea Therapeutics Inc.

  • Pre-clinical findings underscore the potential of APR-1051, a next-generation WEE1 kinase inhibitor, to be a well-tolerated and effective treatment for Cyclin E-overexpressing cancers

    IND for APR-1051 has been cleared; details on planned Phase 1 first in human trial (ACESOT-1051) presented

    ATRN-119, a novel macrocyclic ATR inhibitor, continues to appear safe and well tolerated with no Dose Limiting Toxicities observed in ongoing Phase 1/2a study; preliminary signs of clinical benefit reported; enrollment in the study continues

    DOYLESTOWN, Pa., April 10, 2024 (GLOBE NEWSWIRE) -- Aprea Therapeutics, Inc. (NASDAQ:APRE) ("Aprea", or the "Company"), a clinical-stage biopharmaceutical company focused on precision oncology through synthetic lethality, today released details about four poster presentations at the ongoing American Association of Cancer Research (AACR) Annual Meeting, taking place April 5 to 10, 2024 in San Diego, CA. The posters feature APR-1051, Aprea's next-generation inhibitor of WEE1 kinase, as well as a clinical update on ATRN-119, its novel macrocyclic ATR inhibitor. The Company also presented a poster highlighting a new set of preclinical data in glioblastoma with a next-generation macrocyclic ATR inhibitor, ATRN-333.

    "The four poster presentations at this prestigious conference highlight our growing pipeline and commitment to help cancer patients in need," said Dr. Oren Gilad, President and CEO of Aprea. "We are pleased to share the strong pre-clinical data and future clinical strategy for our promising next-generation WEE1 kinase inhibitor, APR-1051. We are also very excited to provide an encouraging update on the ongoing clinical study of our novel macrocyclic ATR inhibitor, ATRN-119."

    Copies of the posters will be available on the Aprea corporate website here, at the conclusion of the AACR meeting.

    APR-1051

    The novel WEE1i, APR-1051, is a potentially well tolerated and effective treatment for cyclin E-overexpressing cancers

    Lead Author and Presenter:
     
    Molly Hansbarger
    Abstract Number:
     
    7121
     
    • This poster summarizes the pre-clinical data of APR-1051
    • APR-1051 exhibits high potency for WEE1 inhibition in vitro

      • Selectivity is key for success. APR-1051 shows low off-target inhibition of the PLK family of kinases.

        • To measure the potential for off-target inhibition of the PLK family of enzymes, in vitro experiments were conducted to determine the IC50s of APR-1051 vs ZN-c3 (Zentalis Pharmaceuticals)
        • The results showed significantly lower off-targeting of PLK1, PLK2 and PLK3 as indicated by higher IC50 values for APR-1051 compared to ZN-c3.
          IC50 of APR-1051 over IC50 of ZN-c3
          • PLK1: > 150-fold
          • PLK2: > 50-fold
          • PLK3: > 600-fold

    • Off-targeting of PLK1 by other WEE1 inhibitors may compromise the efficacy of these drugs.
    • Off-targeting of the PLK family may increase the risk of producing PLKi-associated adverse effects.

    • Cyclin E as a potential biomarker for APR-1051 treatment
      • APR-1051 demonstrated effectiveness in suppressing the growth of Cyclin E-overexpressing breast and ovarian cancer cell lines.
      • The dose and scheduling of APR-1051 that causes significant suppression of CCNE1-amplified high-grade serous ovarian cancer tumors in mice is well tolerated.
      • Red blood cell and platelet counts remained within non-pathogenic ranges after a 28-day treatment period, consistent with proposed minimal off target PLK1 inhibition
    • APR-1051 will potentially exhibit low cardiotoxicity.
      • Inhibition WEE1 by APR-1051 occurs at an IC50 that is 200-fold lower on average than the IC50 of hERG potassium channel inhibition.
    • Strong evidence for combination therapy
      • APR-1051 was evaluated in combination with Aprea's second-generation ATR inhibitors (ATRN-330 and ATRN-354) in xenografted tumors. The results showed higher anti-tumor activity for the combinations, compared with vehicle or monotherapy.
    • APR-1051 received U.S. FDA clearance for a clinical trial, now with plans to dose the first patient in June 2024

    ASECOT-1051: First-in-human phase 1 study of WEE1 inhibitor APR-1051 in patients with advanced solid tumors harboring cancer-associated gene alterations.

    Presenter:
     
    Nadeem Q. Mirza, M.D., MPH
    Lead author:
     
    Timothy Yap, M.D.
    Abstract Number:
     
    CT196
     
    • This poster summarizes the strategy for ...

    Full story available on Benzinga.com

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    Stock Information
    Company Name: Aprea Therapeutics Inc.
    Stock Symbol: APRE
    Market: NASDAQ
    Website: aprea.com
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