Please use this identifier to cite or link to this item: https://ahro.austin.org.au/austinjspui/handle/1/24827
Title: Lipoprotein apheresis and PCSK9 inhibitors for severe familial hypercholesterolaemia: Experience from Australia and New Zealand.
Austin Authors: Page, Michael M;Ekinci, Elif I ;Burnett, John R;Hooper, Amanda J;Reid, Nicola;Bishop, Warrick;Florkowski, Chris M;Scott, Russell;O'Brien, Richard C ;Watts, Gerald F
Affiliation: Endocrinology
Medicine (University of Melbourne)
Department of Clinical Biochemistry, PathWest Laboratory Medicine, Royal Perth Hospital and Fiona Stanley Hospital, Perth, Western Australia, Australia
School of Medicine, University of Western Australia, Crawley, Western Australia, Australia
Department of Clinical Biochemistry, PathWest Laboratory Medicine, Royal Perth Hospital and Fiona Stanley Hospital, Perth, Western Australia, Australia
Cardiovascular Prevention and Lipid Disorders Clinic, Christchurch Hospital, Christchurch, New Zealand
Calvary Cardiac Centre, Calvary Hospital, Lenah Valley, Tasmania, Australia
Canterbury Health Laboratories, Christchurch, New Zealand
Lipid Disorders Clinic, Cardiovascular Medicine, Royal Perth Hospital, Perth, Western Australia, Australia
School of Medicine, University of Western Australia, Crawley, Western Australia, Australia
Western Diagnostic Pathology, Myaree, Western Australia, Australia
Issue Date: Feb-2021
Date: 2020-09-10
Publication information: Journal of Clinical Apheresis 2021; 36(1): 48-58
Abstract: Severe familial hypercholesterolaemia (FH) causes premature disability and death due to atherosclerotic cardiovascular disease and is refractory to standard lipid-lowering therapies. Lipoprotein apheresis (LA) has long been a standard of care for patients with severe FH, but is invasive, expensive and time-consuming for patients and their caregivers. Newer drug therapies, including the proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibitors, may reduce the need for LA. We audited the records of 16 patients (eight homozygous, eight heterozygous) treated with LA in Australia and New Zealand, 14 of whom subsequently commenced PCSK9 inhibitor therapy. LA was performed by cascade filtration in all centres. LDL-cholesterol was acutely lowered by 69 ± 7% in patients with homozygous FH and by 72 ± 9% in those with heterozygous FH, representing time-averaged reductions of 36 ± 12% and 34 ± 5%, respectively. LA was well-tolerated, and patients reported comparable quality of life to population and disease-related norms. After commencement of PCSK9 inhibitors, four of seven patients with homozygous FH had meaningful biochemical responses, with a reduction in the frequency of LA permitted in one patient and complete cessation in another. Four of seven patients with heterozygous FH were able to be managed without LA after commencing PCSK9 inhibitors. While PCSK9 inhibitors have reduced the need for LA, some patients with severe FH continue to require LA, and will require it for the foreseeable future. However, emerging therapies, including angiopoetin-like 3 inhibitors, may further reduce the need for LA.
URI: https://ahro.austin.org.au/austinjspui/handle/1/24827
DOI: 10.1002/jca.21839
ORCID: 0000-0002-3593-2073
Journal: Journal of Clinical Apheresis
PubMed URL: 32911577
Type: Journal Article
Subjects: PCSK9 inhibitors
familial hypercholesterolaemia
health-related quality of life
lipoprotein apheresis
Appears in Collections:Journal articles

Show full item record

Page view(s)

80
checked on Dec 18, 2024

Google ScholarTM

Check


Items in AHRO are protected by copyright, with all rights reserved, unless otherwise indicated.