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Vol. 40. Núm. 3.
Páginas 225-227 (março 2021)
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Vol. 40. Núm. 3.
Páginas 225-227 (março 2021)
Letter to the Editor
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Lipoprotein(a) in familial hypercholesterolemia: Tips from family history
Lipoproteína (a) na hipercolesterolemia familiar: «truques» de histórias familiares
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Beatrice Dal Pinoa, Francesco Sbranaa,
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francesco.sbrana@ftgm.it

Corresponding author.
, Michele Coceanib, Federico Bigazzia, Tiziana Sampietroa
a Lipoapheresis Unit and Reference Center for Inherited Dyslipidemias, Fondazione Toscana Gabriele Monasterio, Pisa, Italy
b Invasive Cardiology Unit, Fondazione Toscana Gabriele Monasterio, Pisa, Italy
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Dear Editor,

We read with interest the paper by Brandão et al. entitled Lipoprotein(a) as a key target in combined therapeutic approaches for cardiovascular disease1 highlighting, in the era of new lipid-lowering drugs,2,3 the value of Lipoprotein(a) [Lp(a)] as a risk factor for atherosclerotic cardiovascular disease4 and the importance of its measurement in the cascade screening of familial hypercholesterolemia (FH).5,6 We were comforted by these results because we have been dosing Lp(a) at our Institute for this specific purpose for many years now. Indeed, already in the 1980s, the central role of Lp(a) in cardiovascular disease was demonstrated by various lines of research – epidemiology, biochemistry, pathophysiology7 and, unsurprisingly, measurement of Lp(a) has been strongly advocated in FH, as well as in other more frequent forms of dyslipidemia.8

Subsequent studies reinforced the importance of Lp(a), which should be assessed in all patients with premature coronary artery disease (CAD) in the absence of major coronary risk factors. Moreover, Lp(a) levels have been found to have a causal role in CAD and the relationship is so strong that, in some countries (such as Germany), Lp(a)-lowering therapy (i.e. lipoprotein apheresis) is reimbursed by the public health system.9

The paper by Ellis et al. has the merits of unifying the vision of Lp(a) across the Atlantic and draws attention to an argument which, still today, represents a missed opportunity in cardiovascular medicine, especially considering that we finally have the therapeutic means to intervene in patients with elevated Lp(a). In addition, the study provides the impetus to associate cascade screening with personalized therapy, as exemplified by the case of a family cared for at our Institute (Figure 1). In these cases, we were able to obtain an optimal balance between maximally tolerated lipid-lowering therapy, proprotein convertase subtilisin kexin type 9 inhibitors (PCSK9i) and lipoprotein apheresis. It should be borne in mind that PCSK9i therapy can be titrated to maintain adequate LDL-C levels while increasing the administration interval,10 although the effect on Lp(a) levels may be unpredictable.11

Figure 1.

Pedigree of the proband family 1.

The proband (subject III.4) was referred to our Institute after percutaneous coronary intervention and was diagnosed with FH LDL-receptor gene (c.1860G>A) mutation. The other family members were identified by cascade screening and consequently treated. Two cousins with extremely high levels of Lp(a) associated with FH were started on lipoprotein apheresis (subject III.5 had undergone percutaneous coronary intervention, whereas subject III.6 had had a rapid progression of carotid atherosclerosis despite statin therapy). The proband (subject III.4) was treated temporarily with lipoprotein apheresis, which was subsequently replaced with PCSK9i therapy.

Legend: *: Proband; ▴: concomitant spinocerebellar ataxias with hyper-CPK; ATS: peripheral atherosclerosis on carotid vessels; CAD: coronary artery disease; HDL-C: high density lipoprotein cholesterol (mg/dl); LDL-C: low density lipoprotein cholesterol (mg/dl); Lp(a): lipoprotein(a) (mg/dl); TC: total cholesterol (mg/dl); TG: triglycerides (mg/dl); y: years.

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Funding sources

No financial support was received.

Conflicts of interest

The authors have no conflicts of interest to declare.

Acknowledgments

The authors are grateful to Mascia Pianelli and Roberta Luciani for the excellent work in the apheresis unit.

References
[1]
J.A.M. Brandão, L.R. Meireles-Brandão, R. Coelho, et al.
Lipoprotein(a) as a key target in combined therapeutic approaches for cardiovascular disease.
Rev Port Cardiol, 38 (2019), pp. 485-493
[2]
L.D. Colantonio, K.L. Monda, R.S. Rosenson, et al.
Characteristics and cardiovascular disease event rates among African Americans and Whites who meet the further cardiovascular outcomes research with PCSK9 inhibition in subjects with elevated risk (Fourier) trial inclusion criteria.
Cardiovasc Drugs Ther, 33 (2019), pp. 189-199
[3]
H.N. Ginsberg, J. Tuomilehto, G.K. Hovingh, et al.
Impact of age on the efficacy and safety of alirocumab in patients with heterozygous familial hypercholesterolemia.
Cardiovasc Drugs Ther, 33 (2019), pp. 69-76
[4]
H. Tada, M. Takamura, M.A. Kawashiri.
Lipoprotein(a) as an old and new causal risk factor of atherosclerotic cardiovascular disease.
J Atheroscler Thromb, 26 (2019), pp. 583-591
[5]
K.L. Ellis, L. Pérez de Isla, R. Alonso, et al.
Value of measuring lipoprotein(a) during cascade testing for familial hypercholesterolemia.
J Am Coll Cardiol, 73 (2019), pp. 1029-1039
[6]
M.P. Bogsrud, A. Græsdal, D. Johansen, et al.
LDL-cholesterol goal achievement, cardiovascular disease, and attributed risk of Lp(a) in a large cohort of predominantly genetically verified familial hypercholesterolemia.
J Clin Lipidol, 13 (2019), pp. 279-286
[7]
G. Utermann.
The mysteries of lipoprotein(a).
Science, 246 (1989), pp. 904-910
[8]
A. Wiegman, J. Rodenburg, S. de Jongh, et al.
Family history and cardiovascular risk in familial hypercholesterolemia: data in more than 1000 children.
Circulation, 107 (2003), pp. 1473-1478
[9]
J. Leebmann, E. Roeseler, U. Julius, Pro(a)LiFe Study Group, et al.
Lipoprotein apheresis in patients with maximally tolerated lipid-lowering therapy, lipoprotein(a)-hyperlipoproteinemia, and progressive cardiovascular disease: prospective observational multicenter study.
Circulation, 128 (2013), pp. 2567-2576
[10]
T. Sampietro, F. Bigazzi, F. Sbrana, et al.
Personalized regimen for PCSK9 inhibitors: a therapeutic option that maintains efficacy and reduces costs.
J Clin Lipidol, 12 (2018), pp. 1324-1325
[11]
F. Sbrana, F. Bigazzi, B. Dal Pino, et al.
Elusive therapeutic effect of PCSK9 inhibitors on lipoprotein(a) levels.
Ther Apher Dial, 23 (2019), pp. 385-386
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