Familial hypercholesterolaemia: A study of 36 cases with a phenotype of homozygous familiar hypercholesterolaemia

Álvaro J. Ruiz; Luisa Fernanda Patiño; Kelly Amaya; Juan Esteban Gómez; Felipe Ordóñez; Samuel Paternina; Misael Mercado; Harry Pachajoa; Rafael Campo; Gustavo Giraldo; Ravagly Jiménez; Nohora Zuluaga; Jeniffer Monroy; Julián Gil-Forero; Audrey Matallana; Carolina Rivera; Mauricio Coll; William A. Peña-Vargas; Octavio Manjarrez; Juan Martín Toro; Álvaro Barrera; Diego Hoyos; Harold García

doi:10.1016/j.rccar.2019.10.006

Familial hypercholesterolaemia: A study of 36 cases with a phenotype of homozygous familiar hypercholesterolaemia

Título traducido de la contribución: Hipercolesterolemia familiar: serie de 36 casos con fenotipo de hipercolesterolemia familiar homocigótica

Álvaro J. Ruiz, Luisa Fernanda Patiño, Kelly Amaya, Juan Esteban Gómez, Felipe Ordóñez, Samuel Paternina, Misael Mercado, Harry Pachajoa, Rafael Campo, Gustavo Giraldo, Ravagly Jiménez, Nohora Zuluaga, Jeniffer Monroy, Julián Gil-Forero, Audrey Matallana, Carolina Rivera, Mauricio Coll, William A. Peña-Vargas, Octavio Manjarrez, Juan Martín ToroÁlvaro Barrera, Diego Hoyos, Harold García

Producción: Contribución a una revista › Artículo › revisión exhaustiva

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Background: Homozygous familial hypercholesterolemia (HoFH) is characterized for very high levels of cLDL and early cardiovascular disease. Although incidence is low (1/300 000), complications are very severe and can be avoided. Finding and treating this population promptly could reduce mortality. We describe 36 cases in Colombia, where 160 to 200 cases are expected. Results: 36 patients with phenotype of HoHF were identified and treated in a follow-up of 4 years. The mean age was 27 years (24 women). 34 of them had at least 8 points in the FH Dutch Lipid Clinic Criteria (definitive diagnosis) and two had probable diagnosis. A quarter of the cases came from the Colombian North Coast. In molecular tests, 14 were true homozygous for LDLR, 12 were compound heterozygous for LDLR, 2 double heterozygous and one was autosomal recessive; 5 were heterozygous and 2 patients did not authorized genetic test. In true homozygous subjects, the most frequent variant was c.11G>A. 14 patients had coronary disease, 9 carotid stenosis, 8 aortic stenosis and 2 had stroke. 34 patients were on statins (25 rosuvastatin), 30 were receiving ezetimibe, 2 were receiving a PSCK9 inhibitor (evolocumab) and 20 were on lomitapide with mean doses of 12.7 mg. None received lipoprotein apheresis. Medications were very well tolerated. Changes in cLDL after therapy was from 533.7 mg/dL to 245 mg/dL, (54%). Conclusions: Treatment was started in all patients. We found genetic mutations in all patients with genetic tests. The high levels of cLDL mean such a high risk that treatment must be started promptly, even without a genetic test.

Título traducido de la contribución	Hipercolesterolemia familiar: serie de 36 casos con fenotipo de hipercolesterolemia familiar homocigótica
Idioma original	Inglés
Páginas (desde-hasta)	498-507
Número de páginas	10
Publicación	Revista Colombiana de Cardiologia
Volumen	27
N.º	6
DOI	https://doi.org/10.1016/j.rccar.2019.10.006
Estado	Publicada - 01 nov. 2020

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Ruiz, Á. J., Patiño, L. F., Amaya, K., Gómez, J. E., Ordóñez, F., Paternina, S., Mercado, M., Pachajoa, H., Campo, R., Giraldo, G., Jiménez, R., Zuluaga, N., Monroy, J., Gil-Forero, J., Matallana, A., Rivera, C., Coll, M., Peña-Vargas, W. A., Manjarrez, O., ... García, H. (2020). Familial hypercholesterolaemia: A study of 36 cases with a phenotype of homozygous familiar hypercholesterolaemia. Revista Colombiana de Cardiologia, 27(6), 498-507. https://doi.org/10.1016/j.rccar.2019.10.006

@article{f5593310de4445b7919c45c8a7109457,

title = "Familial hypercholesterolaemia: A study of 36 cases with a phenotype of homozygous familiar hypercholesterolaemia",

abstract = "Background: Homozygous familial hypercholesterolemia (HoFH) is characterized for very high levels of cLDL and early cardiovascular disease. Although incidence is low (1/300 000), complications are very severe and can be avoided. Finding and treating this population promptly could reduce mortality. We describe 36 cases in Colombia, where 160 to 200 cases are expected. Results: 36 patients with phenotype of HoHF were identified and treated in a follow-up of 4 years. The mean age was 27 years (24 women). 34 of them had at least 8 points in the FH Dutch Lipid Clinic Criteria (definitive diagnosis) and two had probable diagnosis. A quarter of the cases came from the Colombian North Coast. In molecular tests, 14 were true homozygous for LDLR, 12 were compound heterozygous for LDLR, 2 double heterozygous and one was autosomal recessive; 5 were heterozygous and 2 patients did not authorized genetic test. In true homozygous subjects, the most frequent variant was c.11G>A. 14 patients had coronary disease, 9 carotid stenosis, 8 aortic stenosis and 2 had stroke. 34 patients were on statins (25 rosuvastatin), 30 were receiving ezetimibe, 2 were receiving a PSCK9 inhibitor (evolocumab) and 20 were on lomitapide with mean doses of 12.7 mg. None received lipoprotein apheresis. Medications were very well tolerated. Changes in cLDL after therapy was from 533.7 mg/dL to 245 mg/dL, (54%). Conclusions: Treatment was started in all patients. We found genetic mutations in all patients with genetic tests. The high levels of cLDL mean such a high risk that treatment must be started promptly, even without a genetic test.",

keywords = "Alleles, Familiar hypercholesterolemia, Genetics, LDL cholesterol, Lipids, Mutations, Severe hypercholesterolemia",

author = "Ruiz, {{\'A}lvaro J.} and Pati{\~n}o, {Luisa Fernanda} and Kelly Amaya and G{\'o}mez, {Juan Esteban} and Felipe Ord{\'o}{\~n}ez and Samuel Paternina and Misael Mercado and Harry Pachajoa and Rafael Campo and Gustavo Giraldo and Ravagly Jim{\'e}nez and Nohora Zuluaga and Jeniffer Monroy and Juli{\'a}n Gil-Forero and Audrey Matallana and Carolina Rivera and Mauricio Coll and Pe{\~n}a-Vargas, {William A.} and Octavio Manjarrez and Toro, {Juan Mart{\'i}n} and {\'A}lvaro Barrera and Diego Hoyos and Harold Garc{\'i}a",

note = "Publisher Copyright: {\textcopyright} 2020 Sociedad Colombiana de Cardiolog{\'i}a y Cirug{\'i}a Cardiovascular",

year = "2020",

month = nov,

day = "1",

doi = "10.1016/j.rccar.2019.10.006",

language = "English",

volume = "27",

pages = "498--507",

journal = "Revista Colombiana de Cardiologia",

issn = "0120-5633",

publisher = "Permanyer Publications Ltd",

number = "6",

}

Ruiz, ÁJ, Patiño, LF, Amaya, K, Gómez, JE, Ordóñez, F, Paternina, S, Mercado, M, Pachajoa, H, Campo, R, Giraldo, G, Jiménez, R, Zuluaga, N, Monroy, J, Gil-Forero, J, Matallana, A, Rivera, C, Coll, M, Peña-Vargas, WA, Manjarrez, O, Toro, JM, Barrera, Á, Hoyos, D & García, H 2020, 'Familial hypercholesterolaemia: A study of 36 cases with a phenotype of homozygous familiar hypercholesterolaemia', Revista Colombiana de Cardiologia, vol. 27, n.º 6, pp. 498-507. https://doi.org/10.1016/j.rccar.2019.10.006

TY - JOUR

T1 - Familial hypercholesterolaemia

T2 - A study of 36 cases with a phenotype of homozygous familiar hypercholesterolaemia

AU - Ruiz, Álvaro J.

AU - Patiño, Luisa Fernanda

AU - Amaya, Kelly

AU - Gómez, Juan Esteban

AU - Ordóñez, Felipe

AU - Paternina, Samuel

AU - Mercado, Misael

AU - Pachajoa, Harry

AU - Campo, Rafael

AU - Giraldo, Gustavo

AU - Jiménez, Ravagly

AU - Zuluaga, Nohora

AU - Monroy, Jeniffer

AU - Gil-Forero, Julián

AU - Matallana, Audrey

AU - Rivera, Carolina

AU - Coll, Mauricio

AU - Peña-Vargas, William A.

AU - Manjarrez, Octavio

AU - Toro, Juan Martín

AU - Barrera, Álvaro

AU - Hoyos, Diego

AU - García, Harold

PY - 2020/11/1

Y1 - 2020/11/1

N2 - Background: Homozygous familial hypercholesterolemia (HoFH) is characterized for very high levels of cLDL and early cardiovascular disease. Although incidence is low (1/300 000), complications are very severe and can be avoided. Finding and treating this population promptly could reduce mortality. We describe 36 cases in Colombia, where 160 to 200 cases are expected. Results: 36 patients with phenotype of HoHF were identified and treated in a follow-up of 4 years. The mean age was 27 years (24 women). 34 of them had at least 8 points in the FH Dutch Lipid Clinic Criteria (definitive diagnosis) and two had probable diagnosis. A quarter of the cases came from the Colombian North Coast. In molecular tests, 14 were true homozygous for LDLR, 12 were compound heterozygous for LDLR, 2 double heterozygous and one was autosomal recessive; 5 were heterozygous and 2 patients did not authorized genetic test. In true homozygous subjects, the most frequent variant was c.11G>A. 14 patients had coronary disease, 9 carotid stenosis, 8 aortic stenosis and 2 had stroke. 34 patients were on statins (25 rosuvastatin), 30 were receiving ezetimibe, 2 were receiving a PSCK9 inhibitor (evolocumab) and 20 were on lomitapide with mean doses of 12.7 mg. None received lipoprotein apheresis. Medications were very well tolerated. Changes in cLDL after therapy was from 533.7 mg/dL to 245 mg/dL, (54%). Conclusions: Treatment was started in all patients. We found genetic mutations in all patients with genetic tests. The high levels of cLDL mean such a high risk that treatment must be started promptly, even without a genetic test.

AB - Background: Homozygous familial hypercholesterolemia (HoFH) is characterized for very high levels of cLDL and early cardiovascular disease. Although incidence is low (1/300 000), complications are very severe and can be avoided. Finding and treating this population promptly could reduce mortality. We describe 36 cases in Colombia, where 160 to 200 cases are expected. Results: 36 patients with phenotype of HoHF were identified and treated in a follow-up of 4 years. The mean age was 27 years (24 women). 34 of them had at least 8 points in the FH Dutch Lipid Clinic Criteria (definitive diagnosis) and two had probable diagnosis. A quarter of the cases came from the Colombian North Coast. In molecular tests, 14 were true homozygous for LDLR, 12 were compound heterozygous for LDLR, 2 double heterozygous and one was autosomal recessive; 5 were heterozygous and 2 patients did not authorized genetic test. In true homozygous subjects, the most frequent variant was c.11G>A. 14 patients had coronary disease, 9 carotid stenosis, 8 aortic stenosis and 2 had stroke. 34 patients were on statins (25 rosuvastatin), 30 were receiving ezetimibe, 2 were receiving a PSCK9 inhibitor (evolocumab) and 20 were on lomitapide with mean doses of 12.7 mg. None received lipoprotein apheresis. Medications were very well tolerated. Changes in cLDL after therapy was from 533.7 mg/dL to 245 mg/dL, (54%). Conclusions: Treatment was started in all patients. We found genetic mutations in all patients with genetic tests. The high levels of cLDL mean such a high risk that treatment must be started promptly, even without a genetic test.

KW - Alleles

KW - Familiar hypercholesterolemia

KW - Genetics

KW - LDL cholesterol

KW - Lipids

KW - Mutations

KW - Severe hypercholesterolemia

UR - http://www.scopus.com/inward/record.url?scp=85097173703&partnerID=8YFLogxK

U2 - 10.1016/j.rccar.2019.10.006

DO - 10.1016/j.rccar.2019.10.006

M3 - Article

AN - SCOPUS:85097173703

SN - 0120-5633

VL - 27

SP - 498

EP - 507

JO - Revista Colombiana de Cardiologia

JF - Revista Colombiana de Cardiologia

IS - 6

ER -

Familial hypercholesterolaemia: A study of 36 cases with a phenotype of homozygous familiar hypercholesterolaemia

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