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Related Concept Videos

Targeted Cancer Therapies02:57

Targeted Cancer Therapies

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The targeted cancer therapies, also known as “molecular targeted therapies,” take advantage of the molecular and genetic differences between the cancer cells and the normal cells. It needs a thorough understanding of the cancer cells to develop drugs that can target specific molecular aspects that drive the growth, progression, and spread of cancer cells without affecting the growth and survival of other normal cells in the body.
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Cancer therapies are various modes of treatment, such as surgery, radiation therapy, and chemotherapy that are administered to cancer patients.
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Immunotherapy is a treatment that boosts or manipulates the immune system to fight diseases, including cancer. For instance, by stimulating an immune response through vaccinations against viruses that cause cancers, like hepatitis B virus and human papillomavirus, these diseases can be prevented. Nonetheless, some cancer cells can avoid the immune system due to their rapid mutation and division. The immune response to many cancers involves three phases: elimination, equilibrium, and escape.
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A Mouse Model of Incompletely Resected Soft Tissue Sarcoma for Testing Neoadjuvant Therapies
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Novel Therapeutics in Soft Tissue Sarcoma.

Leonidas Mavroeidis1, Andrea Napolitano1, Paul Huang1

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|January 11, 2025
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Summary
This summary is machine-generated.

Recent advancements in soft tissue sarcoma (STS) therapeutics include FDA-approved targeted therapies and immunotherapies. Overcoming challenges in rare and heterogeneous STS requires better biological understanding and novel drug development strategies.

Keywords:
drug developmentsoft tissue sarcomatherapeuticstreatment

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Area of Science:

  • Oncology
  • Molecular Biology
  • Pharmacology

Background:

  • Soft tissue sarcomas (STS) are a rare and heterogeneous group of cancers.
  • Significant progress has been made in understanding STS molecular characteristics and developing targeted treatments.

Purpose of the Study:

  • To review recent advancements in molecular characterization and therapeutics for soft tissue sarcomas.
  • To highlight novel agents approved by the FDA and investigational treatments for various STS subtypes.

Main Methods:

  • Review of recent FDA approvals for novel agents in STS treatment.
  • Summary of investigational therapies targeting specific molecular alterations and pathways in STS.
  • Discussion of challenges and future directions in STS drug development.

Main Results:

  • Several novel agents, including tyrosine kinase inhibitors (avapritinib, ripretinib), immune checkpoint inhibitors (atezolizumab), and others (nirogacestat, larotrectinib, entrectinib, nab-sirolimus, tazemetostat), have gained FDA approval for specific STS subtypes.
  • Investigational treatments like MDM2 and CDK4/6 inhibitors, further immune checkpoint inhibitors, and PARP inhibitors show promise.
  • Accelerated approval was granted for autologous T-cell therapy (afami-cel) in synovial sarcoma.

Conclusions:

  • Despite challenges posed by rarity and molecular heterogeneity, significant therapeutic progress is being made in soft tissue sarcomas.
  • Future progress hinges on a deeper understanding of STS biology, development of novel compounds for challenging targets (e.g., Proteolysis Targeting Chimeras - PROTACs), innovative clinical trial designs, and industry-academia collaboration.