View Item 

Show simple item record

Gene therapy: Practical aspects of implementation
dc.contributor.authorPipe, Steven W.
dc.contributor.authorReddy, K. Rajender
dc.contributor.authorChowdary, Pratima
dc.date.accessioned2022-06-01T20:28:09Z
dc.date.available2023-06-01 16:28:08en
dc.date.available2022-06-01T20:28:09Z
dc.date.issued2022-05
dc.identifier.citationPipe, Steven W.; Reddy, K. Rajender; Chowdary, Pratima (2022). "Gene therapy: Practical aspects of implementation." Haemophilia 28: 44-52.
dc.identifier.issn1351-8216
dc.identifier.issn1365-2516
dc.identifier.urihttps://hdl.handle.net/2027.42/172792
dc.description.abstractThe first wave of gene therapies for haemophilia submitted for regulatory review utilize a liver-directed approach in which a functional gene copy of factor VIII (FVIII) or factor IX (FIX) is packaged inside a recombinant adeno-associated viral vector (rAAV). Following a single treatment event, these particles are taken up into liver cells, where the rAAV uncoats and delivers the DNA to the nucleus of the cell, where genetic elements that accompany the gene allow for efficient expression and secretion of FVIII or FIX protein into the plasma. An immune response to the vector capsid has been manifest by elevations in common liver enzymes that must be diligently followed postinfusion for weeks and months afterward and if signs of toxicity appear, will trigger a course of immunosuppression. Despite this, the studies have shown that this works in the great majority of individuals and the immunosuppression course is either avoided or short-lived for many. Optimal outcomes in the haemophilia population will be dependent on proper screening assessment and maintenance of liver health prior to consideration of gene therapy, close short-term follow up and implementation of immunomodulatory strategies to identify and manage liver toxicity and preserve durable transgene expression. This review proposes best practices to assist clinical teams with overcoming the challenges this platform of therapy poses to the traditional clinical care models and infrastructure within the haemophilia treatment centres (HTCs) who will be coordinating the patient’s journey through this potentially transformative therapy.
dc.publisherWiley Periodicals, Inc.
dc.subject.otherhaemophilia treatment centre
dc.subject.otherinfrastructure
dc.subject.otherliver health
dc.subject.otherimmunosuppression
dc.subject.othergene therapy
dc.titleGene therapy: Practical aspects of implementation
dc.typeArticle
dc.rights.robotsIndexNoFollow
dc.subject.hlbsecondlevelOncology and Hematology
dc.subject.hlbtoplevelHealth Sciences
dc.description.peerreviewedPeer Reviewed
dc.description.bitstreamurlhttp://deepblue.lib.umich.edu/bitstream/2027.42/172792/1/hae14545.pdf
dc.description.bitstreamurlhttp://deepblue.lib.umich.edu/bitstream/2027.42/172792/2/hae14545_am.pdf
dc.identifier.doi10.1111/hae.14545
dc.identifier.sourceHaemophilia
dc.identifier.citedreferenceMingozzi F, High KA. Overcoming the host immune response to adeno-associated virus gene delivery vectors: the race between clearance, tolerance, neutralization, and escape. Annual Review of Virology. 2017; 4 ( 1 ): 511 - 534.
dc.identifier.citedreferenceMiesbach W, Chowdary P, Coppens M, et al. Delivery of AAV-based gene therapy through haemophilia centres-A need for re-evaluation of infrastructure and comprehensive care: a Joint publication of EAHAD and EHC. Haemophilia. 2021; 27 ( 6 ): 967 - 973.
dc.identifier.citedreferenceMiesbach W, Pasi KJ, Pipe SW, et al. Evolution of haemophilia integrated care in the era of gene therapy: treatment centre’s readiness in United States and EU. Haemophilia. 2021; 27 ( 4 ): 511 - 514.
dc.identifier.citedreferencePipe SW. Delivering on the promise of gene therapy for haemophilia. Haemophilia. 2021; 27 (Suppl 3 ): 114 - 121.
dc.identifier.citedreferencePipe SW, Gonen-Yaacovi G, Segurado OG. Hemophilia A gene therapy: current and next-generation approaches. Expert Opin Biol Ther. 2022: 1 - 17.
dc.identifier.citedreferenceValentino LA, Baker JR, Butler R, et al. Integrated hemophilia patient care via a national network of care centers in the United States: a model for rare coagulation disorders. J Blood Med. 2021; 12: 897 - 911.
dc.identifier.citedreferenceKonkle B, Pierce G, Coffin D, et al. Core data set on safety, efficacy, and durability of hemophilia gene therapy for a global registry: communication from the SSC of the ISTH. J Thromb Haemost. 2020; 18 ( 11 ): 3074 - 3077.
dc.identifier.citedreferenceKonkle BA, Coffin D, Pierce GF, et al. World federation of hemophilia gene therapy registry. Haemophilia. 2020; 26 ( 4 ): 563 - 564.
dc.identifier.citedreferenceMakris M, Calizzani G, Fischer K, et al. EUHASS: the European haemophilia safety surveillance system. Thromb Res. 2011; 127 (Suppl 2 ): S22 - 25.
dc.identifier.citedreferenceNathwani AC, Tuddenham EGD, Rangarajan S, et al. Adenovirus-associated virus vector–mediated gene transfer in hemophilia B. New Engl J Med. 2011; 365 ( 25 ): 2357 - 2365.
dc.identifier.citedreferenceRonzitti G, Gross D-A, Mingozzi F. Human immune responses to Adeno-Associated Virus (AAV) vectors. Front Immunol. 2020; 11 ( 670 ).
dc.identifier.citedreferenceWang D, Tai PWL, Gao G. Adeno-associated virus vector as a platform for gene therapy delivery. Nat Rev Drug Discov. 2019; 18 ( 5 ): 358 - 378.
dc.identifier.citedreferenceBessis N, GarciaCozar FJ, Boissier MC. Immune responses to gene therapy vectors: influence on vector function and effector mechanisms. Gene Therapy. 2004; 11 ( 1 ): S10 - S17.
dc.identifier.citedreferenceCalcedo R, Wilson J. Humoral immune response to AAV. Front Immunol. 2013; 4 ( 341 ).
dc.identifier.citedreferenceMingozzi F, High KA. Immune responses to AAV vectors: overcoming barriers to successful gene therapy. Blood. 2013; 122 ( 1 ): 23 - 36.
dc.identifier.citedreferencePipe S, Leebeek FWG, Ferreira V, Sawyer EK, Pasi J. Clinical considerations for capsid choice in the development of liver-targeted AAV-based gene transfer. Mol Ther Methods Clin Dev. 2019; 15: 170 - 178.
dc.identifier.citedreferenceMonahan PE, Négrier C, Tarantino M, Valentino LA, Mingozzi F. Emerging immunogenicity and genotoxicity considerations of adeno-associated virus vector gene therapy for hemophilia. Journal of Clinical Medicine. 2021; 10 ( 11 ): 2471.
dc.identifier.citedreferenceChu WS, Ng J. Immunomodulation in administration of rAAV: preclinical and clinical adjuvant pharmacotherapies. Frontiers in Immunology. 2021; 12 ( 858 ).
dc.identifier.citedreferenceJiang H, Couto LB, Patarroyo-White S, et al. Effects of transient immunosuppression on adenoassociated, virus-mediated, liver-directed gene transfer in rhesus macaques and implications for human gene therapy. Blood. 2006; 108 ( 10 ): 3321 - 3328.
dc.identifier.citedreferenceMueller C, Berry JD, McKenna-Yasek DM, et al. SOD1 suppression with adeno-associated virus and MicroRNA in familial ALS. New England Journal of Medicine. 2020; 383 ( 2 ): 151 - 158.
dc.identifier.citedreferenceLiu D, Ahmet A, Ward L, et al. A practical guide to the monitoring and management of the complications of systemic corticosteroid therapy. Allergy Asthma Clin Immunol. 2013; 9 ( 1 ): 30.
dc.identifier.citedreferenceChan YK, Wang SK, Chu CJ, et al. Engineering adeno-associated viral vectors to evade innate immune and inflammatory responses. Sci Transl Med. 2021; 13 ( 580 ).
dc.identifier.citedreferenceMeliani A, Boisgerault F, Hardet R, et al. Antigen-selective modulation of AAV immunogenicity with tolerogenic rapamycin nanoparticles enables successful vector re-administration. Nature Commun. 2018; 9 ( 1 ): 4098.
dc.identifier.citedreferenceKim WR, Flamm SL, Di Bisceglie AM, Bodenheimer HC. Public Policy Committee of the American Association for the Study of Liver D. Serum activity of alanine aminotransferase (ALT) as an indicator of health and disease. Hepatology. 2008; 47 ( 4 ): 1363 - 1370.
dc.identifier.citedreferencePrati D, Taioli E, Zanella A, et al. Updated definitions of healthy ranges for serum alanine aminotransferase levels. Ann Intern Med. 2002; 137 ( 1 ): 1 - 10.
dc.identifier.citedreferencePiton A, Poynard T, Imbert-Bismut F, et al. Factors associated with serum alanine transaminase activity in healthy subjects: consequences for the definition of normal values, for selection of blood donors, and for patients with chronic hepatitis C. MULTIVIRC Group. Hepatology. 1998; 27 ( 5 ): 1213 - 1219.
dc.identifier.citedreferenceSalvaggio A, Periti M, Miano L, Tavanelli M, Marzorati D. Body mass index and liver enzyme activity in serum. Clin Chem. 1991; 37 ( 5 ): 720 - 723.
dc.identifier.citedreferenceMathiesen UL, Franzen LE, Fryden A, Foberg U, Bodemar G. The clinical significance of slightly to moderately increased liver transaminase values in asymptomatic patients. Scand J Gastroenterol. 1999; 34 ( 1 ): 85 - 91.
dc.identifier.citedreferenceKim HC, Nam CM, Jee SH, Han KH, Oh DK, Suh I. Normal serum aminotransferase concentration and risk of mortality from liver diseases: prospective cohort study. BMJ. 2004; 328 ( 7446 ): 983.
dc.identifier.citedreferenceLee TH, Kim WR, Benson JT, Therneau TM. Serum aminotransferase activity and mortality risk in a United States community. Hepatology. 2008; 47 ( 3 ): 880 - 887.
dc.identifier.citedreferenceKennedy P, Wagner M, Castera L, et al. Quantitative elastography methods in liver disease: current evidence and future directions. Radiology. 2018; 286 ( 3 ): 738 - 763.
dc.identifier.citedreferenceYen YH, Kuo FY, Chen CH, et al. Ultrasound is highly specific in diagnosing compensated cirrhosis in chronic hepatitis C patients in real world clinical practice. Medicine (Baltimore). 2019; 98 ( 27 ): e16270.
dc.identifier.citedreferenceFesti D, Schiumerini R, Marzi L, et al. Review article: the diagnosis of non-alcoholic fatty liver disease – availability and accuracy of non-invasive methods. Aliment Pharmacol Ther. 2013; 37 ( 4 ): 392 - 400.
dc.identifier.citedreferenceStern C, Castera L. Non-invasive diagnosis of hepatic steatosis. Hepatol Int. 2017; 11 ( 1 ): 70 - 78.
dc.identifier.citedreferenceCassinotto C, Boursier J, de Ledinghen V, et al. Liver stiffness in nonalcoholic fatty liver disease: a comparison of supersonic shear imaging, FibroScan, and ARFI with liver biopsy. Hepatology. 2016; 63 ( 6 ): 1817 - 1827.
dc.identifier.citedreferenceCassinotto C, Lapuyade B, Guiu B, et al. Agreement between 2-dimensional shear wave and transient elastography values for diagnosis of advanced chronic liver disease. Clin Gastroenterol Hepatol. 2020; 18 ( 13 ): 2971 - 2979.
dc.identifier.citedreferenceSingh S, Venkatesh SK, Wang Z, et al. Diagnostic performance of magnetic resonance elastography in staging liver fibrosis: a systematic review and meta-analysis of individual participant data. Clin Gastroenterol Hepatol. 2015; 13 ( 3 ): 440 - 451. e446.
dc.identifier.citedreferenceHouot M, Ngo Y, Munteanu M, Marque S, Poynard T. Systematic review with meta-analysis: direct comparisons of biomarkers for the diagnosis of fibrosis in chronic hepatitis C and B. Aliment Pharmacol Ther. 2016; 43 ( 1 ): 16 - 29.
dc.identifier.citedreferenceNaveau S, Gaude G, Asnacios A, et al. Diagnostic and prognostic values of noninvasive biomarkers of fibrosis in patients with alcoholic liver disease. Hepatology. 2009; 49 ( 1 ): 97 - 105.
dc.identifier.citedreferenceRatziu V, Massard J, Charlotte F, et al. Diagnostic value of biochemical markers (FibroTest-FibroSURE) for the prediction of liver fibrosis in patients with non-alcoholic fatty liver disease. BMC Gastroenterol. 2006; 6: 6.
dc.identifier.citedreferenceLi J, Gordon SC, Rupp LB, et al. The validity of serum markers for fibrosis staging in chronic hepatitis B and C. J Viral Hepat. 2014; 21 ( 12 ): 930 - 937.
dc.identifier.citedreferenceTreeprasertsuk S, Bjornsson E, Enders F, Suwanwalaikorn S, Lindor KD. NAFLD fibrosis score: a prognostic predictor for mortality and liver complications among NAFLD patients. World J Gastroenterol. 2013; 19 ( 8 ): 1219 - 1229.
dc.identifier.citedreferenceChou R, Wasson N. Blood tests to diagnose fibrosis or cirrhosis in patients with chronic hepatitis C virus infection: a systematic review. Ann Intern Med. 2013; 158 ( 11 ): 807 - 820.
dc.identifier.citedreferenceFrerichs FT. In: Hirschwald A, ed. Über den Diabetes. 1884.
dc.working.doiNOen
dc.owningcollnameInterdisciplinary and Peer-Reviewed


Files in this item

Name:
hae14545.pdf
Size:
292.9KB
Format:
PDF
View/Open
Name:
hae14545_am.pdf
Size:
1.151MB
Format:
PDF
View/Open

Show simple item record

Remediation of Harmful Language

The University of Michigan Library aims to describe library materials in a way that respects the people and communities who create, use, and are represented in our collections. Report harmful or offensive language in catalog records, finding aids, or elsewhere in our collections anonymously through our metadata feedback form. More information at Remediation of Harmful Language.

Accessibility

If you are unable to use this file in its current format, please select the Contact Us link and we can modify it to make it more accessible to you.