Emily C. Lisi
Emory University
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Publication
Featured researches published by Emily C. Lisi.
Journal of Genetic Counseling | 2016
Emily C. Lisi; Shawn E. McCandless
Lysosomal storage diseases (LSDs), lysosomal enzyme deficiencies causing multi-system organ damage, have come to the forefront in newborn screening (NBS) initiatives due to new screening technologies and emerging treatments. We developed a qualitative discussion tool to explore opinions of genetic healthcare providers (HCPs) regarding population-based NBS for MPS types 1 and 2, Pompe, Gaucher, Fabry, and Krabbe diseases. Thirty-eight telephone interviews conducted by a single researcher were analyzed and coded for thematic trends. Six major themes emerged: 1) treatment availability and efficacy is crucial; 2) early age of disease onset is important; 3) ambiguity regarding prognosis is undesirable; 4) parents’ ability to make reproductive decisions is seen by some as a benefit of NBS; 5) paucity of resources for follow-up exists; and 6) the decision-making process for adding conditions to mandated NBS is concerning to HCPs. Among the LSDs discussed, Pompe was considered most appropriate, and Krabbe least appropriate, for NBS. MPS1 and MPS2 were overall considered favorably for screening, but MPS1 ranked higher, due to a perception of better efficacy of therapeutic options. Fabry and Gaucher diseases were viewed less favorably due to later age of onset. The themes identified in this study must be addressed by decision-makers in expanding NBS for LSDs and may be applied to many diseases being considered for NBS in the future.
Molecular genetics and metabolism reports | 2015
Elizabeth Stenger; Zoheb B. Kazi; Emily C. Lisi; Michael J. Gambello; Priya S. Kishnani
Enzyme replacement therapy (ERT) has led to a significant improvement in the clinical course of patients with infantile Pompe disease (IPD), an autosomal recessive glycogen storage disorder characterized by the deficiency in lysosomal acid α-glucosidase. A subset of IPD patients mounts a substantial immune response to ERT developing high sustained anti-rhGAA IgG antibody titers (HSAT) leading to the ineffectiveness of this treatment. HSAT have been challenging to treat, although preemptive approaches have shown success in high-risk patients (those who are cross-reactive immunological material [CRIM]-negative). More recently, the addition of bortezomib, a proteasome inhibitor known to target plasma cells, to immunotherapy with rituximab, methotrexate, and intravenous immunoglobulin has shown success at significantly reducing the anti-rhGAA antibody titers in three patients with HSAT. In this report, we present the successful use of a bortezomib-based approach in a CRIM-positive IPD patient with HSAT and the use of a preemptive approach to prevent immunologic response in an affected younger sibling. We highlight the significant difference in clinical course between the two patients, particularly that a pre-emptive approach was simple and effective in preventing the development of high antibody titers in the younger sibling, thus supporting the role of immune tolerance induction (ITI) in the ERT-naïve high-risk setting.
Molecular Genetics and Metabolism | 2016
Emily C. Lisi; Scott Gillespie; Dawn Laney; Nadia Ali
Molecular Genetics and Metabolism | 2017
Brianna Pruniski; Emily C. Lisi; Nadia Ali
Molecular Genetics and Metabolism | 2016
Amanda Hodgkins; Emily C. Lisi; Nadia Ali
Molecular Genetics and Metabolism | 2016
Emily C. Lisi; Allison Foley; Suma P. Shankar
Archive | 2015
Emily C. Lisi; Shawn E. McCandless
Molecular Genetics and Metabolism | 2015
Kathryn B. Sheets; Zoheb B. Kazi; Stephanie DeArmey; Emily C. Lisi; Elizabeth Stenger; Priya S. Kishnani
Molecular Genetics and Metabolism | 2015
Maria L. Keever; Eleanor G. Botha; Emily C. Lisi; Dawn J. Laney; Taylor Harrison; Hong Li
Molecular Genetics and Metabolism | 2015
Valynne Long; Gulshan Sharma; Douglas D. Robertson; Minzhi Xing; Elie Harmouche; Yegor Podgorsky; Dawn Laney; Michael J. Gambello; Emily C. Lisi; Jad Chamieh; Michael R. Terk