The Health Research Authority website uses essential cookies

This site uses session cookies and persistent cookies to improve the content and structure of the site.

By clicking “Accept All Cookies”, you agree to the storing of cookies on this device to enhance site navigation and content, analyse site usage, and assist in our marketing efforts.

By clicking 'See cookie policy' you can review and change your cookie preferences and enable the ones you agree to.

By dismissing this banner, you are rejecting all cookies and therefore we will not store any cookies on this device.

See cookie policy

LTS13632 Long-term phase 2 study of rhASM in ASMD patients

  • Research type

    Research Study

  • Full title

    A Long-Term Study to Assess the Ongoing Safety and Efficacy of Recombinant Human Acid Sphingomyelinase in Patients With Acid Sphingomyelinase Deficiency

  • IRAS ID

    137260

  • Contact name

    Robin Lachmann

  • Contact email

    robin.lachmann@uclh.nhs.uk

  • Sponsor organisation

    Genzyme Corporation

  • Eudract number

    2013-000051-40

  • Research summary

    Niemann Pick B disease (NPB) is a serious and life threatening disorder for which there is no safe and effective treatment to improve the symptoms or reverse the disease course. In this disorder, a genetic defect results in reduced enzyme acid sphingomyelinase (ASM) activity and thus the 50-fold increase in sphingomyelin levels which then accumulates in organs such as the liver, spleen, lung and bone marrow leading to dysfunction. This study is a Phase 2 trial to evaluate the safety and efficacy of long term treatment with an experimental study drug (recombinant human acid sphingomyelinase rhASM), in patients with Niemann Pick disease due to Acid Sphingomyelinase Deficiency (ASMD). Patients who have ASMD do not have enough activity of the enzyme acid sphingomyelinase (ASM), which normally helps the body break down sphingomyelin (an important building block fat for the cell). As time goes by, cells become overloaded with sphingomyelin and are injured, thereby affecting major organs such as the spleen, liver and lungs and leading to easy bruising, difficulty breathing, slow growth in childhood, delayed puberty, fatigue, pain and possibly other symptoms as well. Although the study doctor will discuss other available treatment options with patients prior to consent, there is no specific treatment to date for ASMD. This study is for patients previously entered in the phase 1b and phase 2 studies of rhASM (a form of enzyme replacement therapy) and will assess the long term efficacy and safety of treatment with rhASM. The Patient Information Sheet will acknowledge that whilst it is possible that rhASM may help to improve some aspects of the disease (including decreases in liver and spleen size, increases in haemoglobin and platelet counts, reduction in bleeding and bruising, and improvements in lung disease, breathing and exercise capacity), rhASM is still experimental and thus no benefit can be guaranteed at this stage.

  • REC name

    London - London Bridge Research Ethics Committee

  • REC reference

    13/LO/1522

  • Date of REC Opinion

    16 Dec 2013

  • REC opinion

    Further Information Favourable Opinion

© Copyright HRA 2025
Site by Big Blue Door