GGrantIndex
← Search

Long-Term Follow-Up and Treatment Outcomes for Individuals with Infantile Pompe Disease

$77,781U54FY2017NSNIH

University Of Minnesota, Minneapolis MN

Investigators

Linked publications & trials

Abstract

The availability of enzyme replacement therapy (ERT) with algucosidase alfa (rhGAA, Myozyme?, Lumizyme?) has been commercially available since 2006 and, in general, has improved the natural history for patients with Infantile Pompe Disease (IPD). Cross Reactive Immunologic Material (CRIM) status is a well-appreciated factor influencing clinical outcomes, as patients who are characterized as CRIM-negative (CN) with no residual GAA enzyme activity are at risk to develop a strong immune response against rhGAA resulting in clinical decline and ultimately death despite continued ERT. Additionally, a subset of CRIM-positive (CP) patients also develope high sustained antibody titers (HSAT). We have developed and demonstrated the success of immune modulation prophylactically in CN patients prior to starting ERT, as well as for CN and CP patients in the entrenched setting after the development of HSAT. With such advances in treatment IPD patients are living longer, transforming the clinical course of Pompe disease as we know it. Further investigation is needed to characterize the emerging natural history of IPD survivors and assess the efficacy of immune tolerance induction (ITI) and suppression algorithms. With supplemental support from Genzyme Corporation and the Alice & YT Chen Pediatrics Genetics & Genomics Research Center, continuation of this observational study [LDN6709; Duke IRB Pro00001562] aims to 1) explore clinical response to treatment in CP and CN IPD patients receiving ERT with and without immune suppression regimens through prospective and retrospective data collection; 2) continue to correlate GAA genotype with CRIM status in association with immune responses; and 3) assess efficacy of immune modulation prophylactically in CN IPD, suppression of HSAT in the entrenched setting, as well as assess prophylactic ITI for CP IPD. Continued long-term clinical data collection will help us to gain a better understanding of natural history and treatment outcomes in IPD, which is expected to guide the use or development of new therapeutic interventions for the next generation of IPD patients?the importance of which is underscored by the advent of newborn screening for IPD.

View original record on NIH RePORTER →