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Enzyme Replacement Therapy

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ERT Basics - Enzyme Power-Up

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ERT Applications - Disease Demolishers

ERT is a key therapeutic strategy for several Lysosomal Storage Diseases (LSDs), involving intravenous administration of recombinant human enzymes to restore deficient activity and ameliorate systemic, non-neurological symptoms.

  • ๐Ÿ“Œ Mnemonic for common ERT-treatable LSDs: We Feel Good Playing Music (Fabry, Gaucher, Pompe, MPS).
DiseaseDeficient EnzymeRecombinant Enzyme (Generic Name)Key Clinical Benefits/Targets
Gaucher Disease (Type 1)GlucocerebrosidaseImiglucerase, Velaglucerase alfaโ†“ Hepatosplenomegaly, โ†‘ hematology, โ†“ bone disease
Fabry Diseaseฮฑ-Galactosidase AAgalsidase alfa/betaโ†“ Pain, stabilize renal/cardiac function, โ†“ Gb3 accumulation
Pompe DiseaseAcid ฮฑ-glucosidase (GAA)Alglucosidase alfaโ†‘ Muscle function/survival, โ†“ cardiomyopathy, โ†“ glycogen
MPS I (Hurler/Scheie)ฮฑ-L-IduronidaseLaronidaseโ†“ Organomegaly, โ†‘ mobility, improved respiration, โ†“ GAGs
MPS II (Hunter)Iduronate-2-sulfataseIdursulfaseโ†“ Organomegaly, โ†‘ walking, airway improvement, โ†“ GAGs
MPS VI (Maroteaux-Lamy)Arylsulfatase BGalsulfaseโ†‘ Endurance, โ†“ GAGs, improved joints/growth

โญ Imiglucerase, for Gaucher disease, was one of the pioneering and highly successful ERTs, significantly improving hematological and visceral manifestations.

ERT Realities - Upsides & Hurdles

Upsides (Advantages):

  • Addresses the fundamental cause: the primary enzyme defect.
  • Proven efficacy: Improves key somatic manifestations (e.g., organomegaly, skeletal dysplasia) in many LSDs.
  • Enhances overall quality of life and can significantly โ†‘ patient survival.

Hurdles (Disadvantages & Challenges):

  • High Cost: Extremely expensive, representing a lifelong financial burden.
  • Administration: Requires lifelong, frequent (typically bi-weekly) intravenous (IV) infusions.
  • Immunogenicity:
    • Common development of anti-drug antibodies (ADAs).
    • Neutralizing antibodies (NAbs) can โ†“ efficacy or cause severe infusion reactions.
  • Limited Biodistribution:
    • Poor penetration of the Blood-Brain Barrier (BBB), thus limiting CNS therapeutic effects.
    • Restricted access to poorly vascularized tissues (cornea, bone, cartilage).
    • Strategies to deliver enzymes across the blood-brain barrier
  • Variable Patient Response: Efficacy and outcomes differ among individuals.
  • Infusion-Associated Reactions (IARs): Potential for mild to severe reactions.

Strategies to Overcome Challenges:

  • Immune tolerance induction (ITI) protocols to mitigate ADA responses.
  • Enzyme engineering for enhanced ERTs:
    • PEGylation ($PEG-enzyme$): โ†‘ circulatory half-life, โ†“ immunogenicity.
    • Altered glycosylation: for improved cellular uptake/targeting and reduced immunogenicity.
  • Next-generation ERTs: aiming for improved biodistribution, stability, and lower immunogenicity.

โญ The development of neutralizing antibodies against the recombinant enzyme is a significant concern that can compromise the long-term efficacy of ERT.

Highโ€‘Yield Points - โšก Biggest Takeaways

  • ERT supplies functional enzymes for enzyme deficiencies, mainly Lysosomal Storage Disorders (LSDs).
  • Treats Gaucher, Fabry, Pompe disease, and Mucopolysaccharidoses (MPS).
  • Administered via regular intravenous (IV) infusions, often lifelong.
  • Challenges: High cost, immunogenicity, and poor Blood-Brain Barrier (BBB) penetration.
  • Improves somatic symptoms and organ function but is not curative.
  • Example: Imiglucerase for Gaucher disease.
  • Manages symptoms; does not correct the underlying genetic defect.

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