The Association of Lipoprotein(a) and Stroke Recurrence: A Systematic Review and Meta-Analysis

Article information

J Stroke. 2025;27(2):161-168

Publication date (electronic) : 2025 May 31

doi : https://doi.org/10.5853/jos.2024.04623

¹Second Department of Neurology, “Attikon” University Hospital, School of Medicine, National and Kapodistrian University of Athens, Athens, Greece

²Department of Neurology & Stroke, Eberhard-Karls University of Tübingen, Tübingen, Germany

³Hertie Institute for Clinical Brain Research, Eberhard-Karls University of Tübingen, Tübingen, Germany

⁴Research Unit and Diabetes Center, Second Department of Internal Medicine, “Attikon” University Hospital, School of Medicine, National and Kapodistrian University of Athens, Athens, Greece

⁵Stroke Center, Lisbon Central University Hospital – ULS São José, and Faculdade de Medicina, Universidade de Lisboa, Lisbon, Portugal

⁶Department of Biotechnological and Applied Clinical Sciences, University of L’Aquila, Via Vetoio, Italy

⁷Department of Neurology, University Hospital Basel, University of Basel, Basel, Switzerland

⁸Third Department of Cardiology, Sotiria Thoracic Diseases General Hospital, National and Kapodistrian University of Athens, Athens, Greece

Correspondence: Georgios Tsivgoulis Second Department of Neurology, “Attikon” University Hospital, School of Medicine, National and Kapodistrian University of Athens, Rimini 1, Chaidari, Athens, Greece 12462 Tel: +30 6937178635 E-mail: tsivgoulisgiorg@yahoo.gr

Received 2024 November 2; Revised 2024 December 25; Accepted 2025 February 11.

Abstract

Background and Purpose

Lipoprotein(a) [Lp(a)] is a lipoprotein structurally similar to low-density lipoprotein and is considered a genetically determined risk factor for cardiovascular disease. Although Lp(a) has been linked to ischemic stroke, its role in secondary stroke prevention, particularly in stroke recurrence, remains unclear.

Methods

A systematic search of MEDLINE and Scopus databases was conducted to identify randomized controlled trials (RCTs) and observational studies reporting Lp(a) levels in patients with ischemic stroke or transient ischemic attack. The primary outcome was stroke recurrence, and secondary outcomes included poor functional outcome, all-cause mortality, and recurrent vascular events. Pooled odds ratios (ORs) were calculated using a random-effects model.

Results

A total of 12 studies, including one RCT post hoc analysis and 11 observational studies, comprising 17,903 patients (mean age 63 years, 38% female), were included. Elevated Lp(a) levels were significantly associated with increased stroke recurrence (OR: 1.69; 95% confidence interval [CI]: 1.09–2.63; P=0.020) and poor functional outcome (OR: 2.09; 95% CI: 1.40–3.11; P<0.001). No significant associations were found between Lp(a) levels and all-cause mortality (OR: 2.20; 95% CI: 0.89–5.43; P=0.088) or recurrent vascular events (OR: 2.66; 95% CI: 0.95–7.44; P=0.063).

Conclusion

Elevated Lp(a) levels are linked to increased stroke recurrence and poor functional outcome in stroke patients. Lp(a) may represent a novel therapeutic target in secondary stroke prevention in addition to a promising biomarker.

Keywords: Lipoprotein(a); Ischemic stroke; Stroke recurrence; Functional outcome; Mortality; Systematic review; Meta-analysis

Introduction

Lipoprotein(a) [Lp(a)] is a complex lipoprotein particle structurally similar to low-density lipoprotein cholesterol (LDL-C), distinguished by the presence of apolipoprotein(a), which is covalently bound to apolipoprotein B-100 [1]. Elevated levels of Lp(a) have been recognized as a genetically determined, independent risk factor for cardiovascular disease, including coronary artery disease and ischemic stroke. Its pathophysiological role is thought to arise from both prothrombotic and atherogenic mechanisms, contributing to plaque instability, thrombosis, and vascular inflammation [2].

Previous studies have demonstrated an association between increased Lp(a) levels and adverse cardiovascular outcomes, particularly among patients with coronary artery disease [3,4]. Furthermore, high Lp(a) levels are considered a risk factor for ischemic stroke, particularly in younger individuals and in patients without traditional vascular risk factors [5]. However, the clinical relevance of elevated Lp(a) in secondary stroke prevention, specifically its role in stroke recurrence, remains unclear.

In recent years, there has been growing interest in therapeutics specifically targeting Lp(a) levels. Novel agents, including antisense oligonucleotides and small interfering RNA-based therapies, have shown promising results in significantly reducing plasma Lp(a) concentrations in early-phase clinical trials [6]. These therapies work by selectively inhibiting the hepatic production of apolipoprotein(a), thereby lowering circulating Lp(a) levels by up to 80%–90%. Ongoing large-scale randomized controlled trials (RCTs) are evaluating whether such reductions can translate into improved cardiovascular and cerebrovascular outcomes, potentially establishing Lp(a) as not only a biomarker but also a modifiable risk factor.

In view of the former considerations, we conducted a systematic review and meta-analysis, including all available randomized and observational evidence, evaluating the role of Lp(a) in stroke prognosis and, more specifically, in stroke recurrence among patients with ischemic stroke or transient ischemic attack.

Methods

Standard protocol approvals, registrations, and patient consents

The prespecified protocol for this systematic review and meta-analysis has been registered in the International Prospective Register of Systematic Reviews (PROSPERO; registration ID: CRD42024603931) and adheres to the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) [7] and the Meta-Analysis of Observational Studies in Epidemiology (MOOSE) reporting guidelines [8].

Data sources, searches, and study selection

A systematic literature search was conducted to identify eligible studies (RCTs, observational cohort studies, or individual patient data meta-analysis of studies) including adult patients with ischemic stroke or transient ischemic attack for whom Lp(a) levels were measured at baseline. Patients with elevated levels of Lp(a) were compared to those with low levels of Lp(a). Reporting of any of the outcomes of interest as outlined below was required for studies to be considered eligible for inclusion. The literature search was performed independently by three reviewers (LP, KM, MIS). The electronic databases MEDLINE and Scopus were searched, using search strings that included the terms “lipoprotein(a)” and “stroke recurrence.” Studies published in English were considered eligible. Our search spanned from the inception of each database to October 20, 2024.

Studies without a control arm, case series, and case reports were excluded. Commentaries, editorials, and narrative reviews were also discarded. In case of studies with duplicate data, the most recent study, further accounting for the number of included patients and outcome reporting, was retained, while the rest were excluded. All retrieved studies were independently assessed by three reviewers (LP, KM, MIS), resolving any disagreements through discussion with the corresponding author (GT).

Quality control, bias assessment, and data extraction

Two reviewers (LP and KM) independently assessed the quality control and bias assessment among eligible studies employing the revised Cochrane Risk-of-Bias tool (RoB 2) for RCTs [9] and the Risk Of Bias In Non-randomized Studies of Exposures (ROBINS-E) tool for observational studies [10]. Any disagreements were settled by consensus after discussion with the corresponding author (GT). Structured forms, which included trial names, year of publication, period of enrollment, patient sample, patients’ characteristics, and outcomes of interest, were used for data extraction.

Outcomes

The primary outcome of interest was stroke recurrence at follow-up, including ischemic stroke, hemorrhagic stroke, any stroke, or transient ischemic attack, as defined by each study. Poor functional outcome, as defined by each study based on dichotomized modified Rankin Scale (mRS) scores (0–2 vs. 3–6 & 0–1 vs. 2–6), all-cause mortality, and recurrent vascular events at follow-up were evaluated as secondary outcomes of interest.

Statistical analysis

For the pairwise meta-analysis, we calculated the corresponding odds ratios (OR) with 95% confidence intervals (CI) for each dichotomous outcome of interest, for the comparison of outcome events among patients with high Lp(a) levels versus those with low Lp(a) levels. Sensitivity analyses were conducted to address variations in outcome definitions by excluding studies with differing definitions. Furthermore, a subgroup analysis was performed for the primary outcome after stratification according to trial setting and population (i.e., Chinese vs. non-Chinese). Baseline characteristics were described using pooled proportions (after the implementation of the variance-stabilizing double arcsine transformation) for categorical variables and mean values for continuous variables. For studies reporting continuous outcomes in median values and corresponding interquartile ranges, the sample mean and standard deviation were estimated using the quantile estimation method [11]. The random-effects model (DerSimonian and Laird 1986) was used to calculate the pooled estimates [12]. The threshold for statistical significance for the above analyses was set at a two-sided P-value of <0.05. Heterogeneity was assessed with the I² and Cochran Q statistics. For the qualitative interpretation of heterogeneity, I² values <25%, between 25%–50%, and >50% were considered to represent low, moderate, and significant heterogeneity, respectively. The significance level for the Q statistic was set at 0.1. The above statistical analyses were performed using the R software version 3.5.0 (package: meta; R Foundation for Statistical Computing, Vienna, Austria) [13].

Data availability statement

All data generated or analyzed during this study are included in this article and its supplementary information files.

Results

Literature search and included studies

The flow diagram for the selection and inclusion of studies in this systematic review is presented in Figure 1. After excluding duplicates, the systematic literature database search yielded a total of 1,028 records. Following the initial screening process, the full texts of 36 records were retrieved. After reading the full-text articles, 24 records were further excluded. Finally, 12 eligible studies (one post hoc analysis of an RCT and 11 observational studies) (Table 1) [14-25] were included in the systematic review and meta-analysis, comprising a total of 17,903 ischemic stroke patients for whom Lp(a) was measured at baseline. Included patients had a mean age of 63 years (Supplementary Figure 1), and 38% were of female sex (Supplementary Figure 2). The majority of the cases presented moderate stroke (mean National Institutes of Health Stroke Scale [NIHSS] score: 7) (Supplementary Figure 3), of which 25% received intravenous thrombolysis and 13% endovascular treatment (Supplementary Figure 4). Twenty-nine percent of the cases were attributed to large-artery atherosclerosis (Supplementary Figure 5), and the mean baseline Lp(a) levels were 34.4 mg/dL (Supplementary Figure 6).

Figure 1.

Flowchart of the systematic review.

Table 1.

Characteristics of studies included in the systematic review and meta-analysis

Quality control of included studies

There was no significant bias detected in any of the quality domains assessed for the study of Chemello et al.,16 which was the only post hoc analysis of an RCT included in this systematic review (Supplementary Figure 7). The majority of the observational studies presented a moderate risk of bias (Supplementary Figure 8), mainly due to unblinded outcome measurements and losses to follow-up, with a lesser contribution from selection bias (inclusion of ischemic stroke patients with diabetes or under statin treatment) and reporting bias (incomplete reporting of outcome data). Only two of the observational studies were graded as “low risk of bias” in all domains.

Quantitative analyses

Regarding the overall effect for the primary outcome of interest, increased levels of Lp(a) were associated with stroke recurrence (OR: 1.69; 95% CI: 1.09–2.63; P=0.020; 5 studies; I²=87%; P for Cochran Q<0.01) (Figure 2). A sensitivity analysis was further conducted to ensure homogeneity of stroke recurrence definition, by excluding the study of Chemello et al.16 that had a more inclusive definition for stroke recurrence taking into account not only ischemic stroke, hemorrhagic stroke, or transient ischemic attack, but also cases with carotid revascularization. In the sensitivity analysis, high Lp(a) levels were again significantly associated with stroke recurrence at follow-up (OR: 2.28; 95% CI: 1.23–4.21; P=0.008; 4 studies; I²=84%; P for Cochran Q<0.01) (Supplementary Figure 9). After stratification for trial setting and population, there were no significant subgroup differences for the primary outcome among studies that included Chinese versus non-Chinese patients (P for subgroup differences =0.82) (Supplementary Figure 10).

Figure 2.

Forest plot presenting the odds ratio of stroke recurrence among patients with high Lp(a) compared to patients with low Lp(a). Lp(a), lipoprotein(a); IV, inverse variance; CI, confidence interval.

Regarding the secondary outcomes of interest, high Lp(a) levels were associated with increased odds of poor functional outcome at follow-up (OR: 2.09; 95% CI: 1.40–3.11; P<0.001; 5 studies; I²=77%; P for Cochran Q<0.01) (Figure 3). During sensitivity analysis, the study of Chakraborty et al.15 that defined poor functional outcome as mRS scores of 2–6 was excluded to ensure the homogeneity of definition (i.e., the rest of the studies used the dichotomized mRS score of 3–6 to define poor functional outcome). This sensitivity analysis confirmed similar results (OR: 1.96; 95% CI: 1.29–2.97; P=0.002; 4 studies; I²=79%; P for Cochran Q<0.01) (Supplementary Figure 11).

Figure 3.

Forest plot presenting the odds ratio of poor functional outcomes among patients with high Lp(a) compared to patients with low Lp(a). Lp(a), lipoprotein(a); IV, inverse variance; CI, confidence interval.

Furthermore, high Lp(a) levels were not associated with mortality (OR: 2.20; 95% CI: 0.89–5.43; P=0.088; 3 studies; I²=66%; P for Cochran Q=0.05) (Figure 4). Finally, there was no association between Lp(a) levels and recurrent vascular events (OR: 2.66; 95% CI: 0.95–7.44; P=0.063; 3 studies; I²=86%; P for Cochran Q<0.01) (Figure 5).

Figure 4.

Forest plot presenting the odds ratio of mortality among patients with high Lp(a) compared to patients with low Lp(a). Lp(a), lipoprotein(a); IV, inverse variance; CI, confidence interval.

Figure 5.

Forest plot presenting the odds ratio of recurrent vascular events among patients with high Lp(a) compared to patients with low Lp(a). Lp(a), lipoprotein(a); IV, inverse variance; CI, confidence interval.

Discussion

This systematic review and meta-analysis demonstrates that elevated Lp(a) levels are associated with higher odds of recurrent stroke and poor functional outcome among patients with ischemic stroke. However, no significant association was observed between Lp(a) levels and mortality or recurrent vascular events, suggesting that the impact of Lp(a) may be more specific to certain post-stroke outcomes.

The observed association between Lp(a) and stroke recurrence may be attributed to the promotion of both atherogenic and thrombotic processes through the structural similarity of Lp(a) to LDL-C and plasminogen, contributing to plaque formation, vascular inflammation, and impaired fibrinolysis [26,27]. These mechanisms may increase the risk of vascular events, particularly in cerebral arteries. In addition, the strong association of higher Lp(a) levels with large artery atherosclerotic stroke, independent of vascular risk factors, may also partially explain our study findings, since large-artery atherosclerosis is the stroke subtype carrying the highest risk of stroke recurrence [28]. Notably, elevated Lp(a) levels have been linked to large-artery atherosclerosis-associated stroke compared to other subtypes, as previously demonstrated [14]. However, there is insufficient data to explore a potential interaction of large-artery atherosclerosis on the association between Lp(a) and stroke outcomes.

Furthermore, higher Lp(a) levels may lead to greater stroke severity, potentially explaining the association with unfavorable functional outcomes. In fact, a positive correlation between NIHSS and Lp(a) has been shown by previous studies [15,18,22,25]. However, the association of Lp(a) with unfavorable outcomes and mortality persisted even after adjustment for baseline NIHSS [22,25].

Despite its potential clinical relevance, current guidelines offer limited recommendations regarding Lp(a) management. The 2019 European Society of Cardiology/European Atherosclerosis Society (ESC/EAS) guidelines recommend measuring Lp(a) at least once in individuals at high cardiovascular risk, especially those with a family history of premature cardiovascular disease or recurrent events despite optimal LDL-C-lowering therapy [29]. Similarly, a recent focused update to the 2019 National Lipid Association scientific statement also recognizes Lp(a) as an important biomarker to refine cardiovascular risk assessment [30]. However, no clear guidance exists on the management of elevated Lp(a) levels specifically for secondary stroke prevention.

Traditionally, stroke prevention strategies have focused on reducing LDL-C levels through statin therapy. While LDL-C reduction is essential, our findings highlight the importance of also considering Lp(a) as a potential therapeutic target [16,17]. Nevertheless, it is crucial to recognize that the association between Lp(a) and stroke recurrence, as demonstrated in our meta-analysis, does not imply causation. Ongoing research, including RCTs investigating Lp(a)-targeting therapies (e.g., antisense oligonucleotides and small interfering RNA), may clarify whether lowering Lp(a) may improve long-term outcomes after stroke [31].

The primary strength of this systematic review lies in its comprehensive analysis of all available studies to date that evaluate the association between baseline Lp(a) and stroke outcomes. In total, our meta-analysis encompasses more than 17,000 ischemic stroke patients, offers a broader perspective, and helps contextualize the findings of individual studies. While another systematic review on Lp(a) and stroke has recently been published [32], several limitations restrict the generalizability of its findings, including a narrower focus on only functional outcomes, a smaller sample size, and an overrepresentation of studies conducted in China.

Nonetheless, this study has several limitations that should be acknowledged. First, the vast majority of the included studies were observational, which inherently limits the strength of the evidence due to potential confounding and bias. Second, the observational studies included in this review were found to have moderate risk of bias, primarily due to unblinded outcome assessments and missing data, which could have affected the results. Third, significant heterogeneity was detected in the analysis of all outcomes, likely due to variations in study design, patient populations, and definitions of outcomes. However, in a subgroup analysis stratifying for trial setting and population, there were no differences among studies including Chinese versus non-Chinese patients. Fourth, the present analyses were not adjusted for vascular risk factors, acute reperfusion treatments, and underlying stroke subtypes. However, sensitivity analyses confirmed the robustness of the primary findings, reinforcing the consistency of the results.

Conclusions

In conclusion, while our meta-analysis indicates that elevated Lp(a) levels are associated with stroke recurrence and poor functional outcomes, further research, particularly through well-designed RCTs, is needed to establish causal relationships and guide the development of targeted interventions for Lp(a) management in patients with ischemic stroke.

Supplementary materials

Supplementary materials related to this article can be found online at https://doi.org/10.5853/jos.2024.04623.

Supplementary Figure 1.

Forest plot presenting the mean age (in years) among included patients. IV, inverse variance; CI, confidence interval; SD, standard deviation.

jos-2024-04623-Supplementary-Fig-1,2,3.pdf

Supplementary Figure 2.

Forest plot presenting the pooled proportion of female sex among included patients. IV, inverse variance; CI, confidence interval.

jos-2024-04623-Supplementary-Fig-1,2,3.pdf

Supplementary Figure 3.

Forest plot presenting the mean NIHSS score among included patients. IV, inverse variance; CI, confidence interval; SD, standard deviation; NIHSS, National Institutes of Health Stroke Scale.

jos-2024-04623-Supplementary-Fig-1,2,3.pdf

Supplementary Figure 4.

Forest plot presenting the pooled proportion of patients receiving intravenous thrombolysis (A) and endovascular treatment (B). IV, inverse variance; CI, confidence interval.

jos-2024-04623-Supplementary-Fig-4,5,6.pdf

Supplementary Figure 5.

Forest plot presenting the pooled proportion of patients with LAA-associated stroke. IV, inverse variance; CI, confidence interval; LAA, large-artery atherosclerosis.

jos-2024-04623-Supplementary-Fig-4,5,6.pdf

Supplementary Figure 6.

Forest plot presenting the mean baseline lipoprotein(a) levels among included patients. IV, inverse variance; CI, confidence interval.

jos-2024-04623-Supplementary-Fig-4,5,6.pdf

Supplementary Figure 7.

Traffic light plot (A) and summary plot (B) presenting the quality assessment for the post hoc analysis of a randomized controlled clinical trial using the revised Cochrane Risk-of-Bias tool (RoB 2).

jos-2024-04623-Supplementary-Fig-7,8.pdf

Supplementary Figure 8.

Traffic light plot (A) and summary plot (B) presenting the quality assessment of the included observational studies using the Risk Of Bias In Non-randomized Studies of Exposures (ROBINS-E) tool.

jos-2024-04623-Supplementary-Fig-7,8.pdf

Supplementary Figure 9.

Forest plot presenting the odds ratio of stroke recurrence among patients with high Lp(a) compared to patients with low Lp(a), during sensitivity analysis excluding the study of Chemello et al. [16] IV, inverse variance; CI, confidence interval; Lp(a), lipoprotein(a).

jos-2024-04623-Supplementary-Fig-9,10,11.pdf

Supplementary Figure 10.

Forest plot presenting the odds ratio of stroke recurrence among patients with high Lp(a) compared to patients with low Lp(a), after stratification according to trial setting and population (i.e., Chinese vs. non-Chinese). IV, inverse variance; CI, confidence interval; Lp(a), lipoprotein(a).

jos-2024-04623-Supplementary-Fig-9,10,11.pdf

Supplementary Figure 11.

Forest plot presenting the odds ratio of poor functional outcomes among patients with high Lp(a) compared to patients with low Lp(a), during sensitivity analysis excluding the study of Chakraborty et al. [15] IV, inverse variance; CI, confidence interval; Lp(a), lipoprotein(a).

jos-2024-04623-Supplementary-Fig-9,10,11.pdf

Notes

Funding statement

None

Conflicts of interest

The authors have no financial conflicts of interest.

Author contribution

Conceptualization: GT. Study design: LP, GT. Methodology: LP, KM, MIS, GT. Data collection: LP, KM, MIS, GT. Investigation: LP, KM, MIS, GT. Statistical analysis: LP, GT. Writing—original draft: LP, GT. Writing—review & editing: KM, MIS, AT, SG, VL, DAS, SS, MK, GS. Approval of final manuscript: all authors.

References

1. Schmidt K, Noureen A, Kronenberg F, Utermann G. Structure, function, and genetics of lipoprotein (a). J Lipid Res 2016;57:1339–1359.

2. Duarte Lau F, Giugliano RP. Lipoprotein(a) and its significance in cardiovascular disease: a review. JAMA Cardiol 2022;7:760–769.

3. Zhang B, Xu Y, Huang X, Sun T, Ma M, Chen Z, et al. Lipoprotein(a) as a novel biomarker for predicting adverse outcomes in ischemic heart failure. Front Cardiovasc Med 2024;11:1466146.

4. Bittner VA, Schwartz GG, Bhatt DL, Chua T, De Silva HA, Diaz R, et al. Alirocumab and cardiovascular outcomes according to sex and lipoprotein(a) after acute coronary syndrome: a report from the ODYSSEY OUTCOMES study. J Clin Lipidol 2024;18:e548–e561.

5. Koh MY, Toh KZ, Loh ED, Teo YN, Joon KC, Tan QX, et al. Association of elevated lipoprotein(a) levels with ischemic stroke in young patients - a systematic review and meta-analysis. J Stroke Cerebrovasc Dis 2024;33:107960.

6. Sosnowska B, Surma S, Banach M. Targeted treatment against lipoprotein (a): the coming breakthrough in lipid lowering therapy. Pharmaceuticals (Basel) 2022;15:1573.

7. Page MJ, McKenzie JE, Bossuyt PM, Boutron I, Hoffmann TC, Mulrow CD, et al. The PRISMA 2020 statement: an updated guideline for reporting systematic reviews. BMJ 2021;372:n71.

8. Stroup DF, Berlin JA, Morton SC, Olkin I, Williamson GD, Rennie D, et al. Meta-analysis Of Observational Studies in Epidemiology: a proposal for reporting. JAMA 2000;283:2008–2012.

9. Sterne JAC, Savovic´ J, Page MJ, Elbers RG, Blencowe NS, Boutron I, et al. RoB 2: a revised tool for assessing risk of bias in randomised trials. BMJ 2019;366:l4898.

10. Higgins JPT, Morgan RL, Rooney AA, Taylor KW, Thayer KA, Silva RA, et al. A tool to assess risk of bias in non-randomized follow-up studies of exposure effects (ROBINS-E). Environ Int 2024;186:108602.

11. McGrath S, Zhao X, Steele R, Thombs BD, Benedetti A, ; DEPRESsion Screening Data (DEPRESSD) Collaboration. Estimating the sample mean and standard deviation from commonly reported quantiles in meta-analysis. Stat Methods Med Res 2020;29:2520–2537.

12. DerSimonian R, Laird N. Meta-analysis in clinical trials revisited. Contemp Clin Trials 2015;45:139–145.

13. Balduzzi S, Rücker G, Schwarzer G. How to perform a metaanalysis with R: a practical tutorial. Evid Based Ment Health 2019;22:153–160.

14. Arnold M, Schweizer J, Nakas CT, Schütz V, Westphal LP, Inauen C, et al. Lipoprotein(a) is associated with large artery atherosclerosis stroke aetiology and stroke recurrence among patients below the age of 60 years: results from the BIOSIGNAL study. Eur Heart J 2021;42:2186–2196.

15. Chakraborty B, Vishnoi G, Goswami B, Gowda SH, Chowdhury D, Agarwal S. Lipoprotein(a), ferritin, and albumin in acute phase reaction predicts severity and mortality of acute ischemic stroke in North Indian Patients. J Stroke Cerebrovasc Dis 2013;22:e159–e167.

16. Chemello K, Gallo A, Guedon AF, Techer R, Croyal M, Swietek MJ, et al. Lipoprotein(a): a residual cardiovascular risk factor in statin-treated stroke survivors: insights from the SPARCL trial. JACC Adv 2023;2:100557.

17. Dong W, Zhong X, Yuan K, Miao M, Zhai Y, Che B, et al. Lipoprotein(a) and functional outcome of acute ischemic stroke when discordant with low-density lipoprotein cholesterol. Postgrad Med J 2023;99:1160–1166.

18. Hong XW, Wu DM, Lu J, Zheng YL, Tu WJ, Yan J. Lipoprotein (a) as a predictor of early stroke recurrence in acute ischemic stroke. Mol Neurobiol 2018;55:718–726.

19. Jiang X, Xu J, Hao X, Xue J, Li K, Jin A, et al. Elevated lipoprotein(a) and lipoprotein-associated phospholipase A2 are associated with unfavorable functional outcomes in patients with ischemic stroke. J Neuroinflammation 2021;18:307.

20. Lange KS, Nave AH, Liman TG, Grittner U, Endres M, Ebinger M. Lipoprotein(a) levels and recurrent vascular events after first ischemic stroke. Stroke 2017;48:36–42.

21. Sanchez Muñoz-Torrero JF, Rico-Martín S, Álvarez LR, Aguilar E, Alcalá JN, Monreal M, et al. Lipoprotein (a) levels and outcomes in stable outpatients with symptomatic artery disease. Atherosclerosis 2018;276:10–14.

22. Wang H, Zhao J, Gui Y, Yan H, Yan Z, Zhang P, et al. Elevated lipoprotein (a) and risk of poor functional outcome in Chinese patients with ischemic stroke and type 2 diabetes. Neurotox Res 2018;33:868–875.

23. Wang L, Liu L, Zhao Y, Chu M, Teng J. Lipoprotein(a) and residual vascular risk in statin-treated patients with first acute ischemic stroke: a prospective cohort study. Front Neurol 2022;13:1004264.

24. Xue J, Xiang Y, Jiang X, Jin A, Hao X, Li K, et al. The joint association of lipoprotein(a) and lipoprotein-associated phopholipase A2 with the risk of stroke recurrence. J Clin Lipidol 2024;18:e729–e737.

25. Zhang W, Zhang XA. Prognostic value of serum lipoprotein(a) levels in patients with acute ischemic stroke. Neuroreport 2014;25:262–266.

26. Lampsas S, Xenou M, Oikonomou E, Pantelidis P, Lysandrou A, Sarantos S, et al. Lipoprotein(a) in atherosclerotic diseases: from pathophysiology to diagnosis and treatment. Molecules 2023;28:969.

27. Kosmas CE, Bousvarou MD, Papakonstantinou EJ, Zoumi EA, Rallidis LS. Lipoprotein (a) and cerebrovascular disease. J Int Med Res 2024;52

28. Rudin S, Kriemler L, Dittrich TD, Zietz A, Schweizer J, Arnold M, et al. Lipoprotein(a) as a blood marker for large artery atherosclerosis stroke etiology: validation in a prospective cohort from a Swiss stroke center. Swiss Med Wkly 2024;154:3633.

29. Mach F, Baigent C, Catapano AL, Koskinas KC, Casula M, Badimon L, et al. 2019 ESC/EAS Guidelines for the management of dyslipidaemias: lipid modification to reduce cardiovascular risk: The Task Force for the management of dyslipidaemias of the European Society of Cardiology (ESC) and European Atherosclerosis Society (EAS). Eur Heart J 2020;41:111–188.

30. Koschinsky ML, Bajaj A, Boffa MB, Dixon DL, Ferdinand KC, Gidding SS, et al. A focused update to the 2019 NLA scientific statement on use of lipoprotein(a) in clinical practice. J Clin Lipidol 2024;18:e308–e319.

31. Wulff AB, Nordestgaard BG, Langsted A. Novel therapies for lipoprotein(a): update in cardiovascular risk estimation and treatment. Curr Atheroscler Rep 2024;26:111–118.

32. Liu H, Li B, Lu T, Chen C, Xiong X, Li X, et al. Impact of elevated lipoprotein(a) levels on the functional outcomes of ischemic stroke patients: a systematic review and meta-analysis. Eur J Neurol 2024;31:e16501.

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Table 1.

Characteristics of studies included in the systematic review and meta-analysis

Authors (yr)	Design	Duration	Included patients	Follow-up duration	Lipoprotein(a) cut-off (mg/dL)	Outcomes of interest
Arnold et al. [14] (2021)	Prospective, observational, multi-center cohort study, Europe	Oct 2014–Oct 2017	1,759 IS (258 LAA and 1,500 non-LAA)	1 year	40	- Stroke recurrence: composite of ischemic stroke and transient ischemic attack
Chakraborty et al. [15] (2012)	Prospective, observational, single-center cohort study, India	Not reported	100 IS	6 months	77	- Mortality
Chakraborty et al. [15] (2012)		Not reported	100 IS	6 months	77	- Poor functional outcome (mRS 2–6)
Chemello et al. [16] (2023)	Post hoc analysis of randomized-controlled clinical trial (SPARCL trial)	Sep 1998–Mar 2001	2,814 IS/TIA	6 years	33.6	- Stroke recurrence: composite of cerebrovascular events (including ischemic stroke, hemorrhagic stroke, transient ischemic attack, and carotid revascularization)
Chemello et al. [16] (2023)		Sep 1998–Mar 2001	2,814 IS/TIA	6 years	33.6	- Ischemic stroke
Dong et al. [17] (2023)	Prospective, observational, multi-center cohort study, China	Jun 2011–Dec 2013	973 IS (505 LAA and 468 non-LAA)	6 months	25.9	- Poor functional outcome (mRS 3–6)
Dong et al. [17] (2023)		Jun 2011–Dec 2013	973 IS (505 LAA and 468 non-LAA)	6 months	25.9	- Mortality
Hong et al. [18] (2016)	Prospective, observational, two-center cohort study, China	Dec 2015–Mar 2016	203 IS (46 LAA and 157 non-LAA)	3 months	30	- Stroke recurrence excluding transient ischemic attack
Jiang et al. [19] (2021)	Third China National Stroke Registry	Aug 2015–Mar 2018	9,709 IS (2,488 LAA and 7,221 non-LAA)	3 months & 1 year	35.8	- Poor functional outcome (mRS 3–6)
Lange et al. [20] (2017)	Prospective, observational, multi-center cohort study, Germany	Jan 2009–Aug 2014	250 IS (54 LAA and 196 non-LAA)	1 year	30	- Recurrent vascular event: composite vascular end point of ischemic stroke, transient ischemic attack, myocardial infarction, nonelective coronary revascularization, and cardiovascular death
Sanchez Muñoz-Torrero et al. [21] (2018)	Prospective, observational, multi-center cohort study, Spain	Mar 2013–Dec 2016	441 IS/TIA	Mean of 36 months	30	- Ischemic stroke recurrence
Sanchez Muñoz-Torrero et al. [21] (2018)		Mar 2013–Dec 2016	441 IS/TIA	Mean of 36 months	30	- Recurrent vascular event: composite of myocardial infarction, ischemic stroke and limb ambutation
Wang et al. [22] (2017)	Prospective, observational, single-center cohort study, China	Not reported	232 IS (50 LAA and 182 non-LAA)	3 months	30	- Poor functional outcome (mRS 3–6)
Wang et al. [22] (2017)		Not reported	232 IS (50 LAA and 182 non-LAA)	3 months	30	- Mortality
Wang et al. [23] (2022)	Retrospective, observational, single-center cohort study, China	Oct 2018–Sep 2020	303 IS (144 LAA and 159 non-LAA)	2 years	30	- Recurrent vascular event: composite of acute ischemic stroke, transient ischemic attack, myocardial infarction and coronary revascularization
Xue et al. [24] (2024)	Third China National Stroke Registry	Aug 2015–Mar 2018	10,675 IS/TIA (2,702 LAA and 7,973 non-LAA)	1 year	50	- Stroke recurrence: composite of ischemic stroke and hemorrhagic stroke
Zhang et al. [25] (2014)	Prospective, observational, single-center cohort study, China	Not reported	153 IS	Discharge	30	- Poor functional outcome (mRS 3–6)

IS, ischemic stroke; LAA, large-artery atherosclerosis; TIA, transient ischemic attack; mRS, modified Rankin Scale; SPARCL trial, Stroke Prevention by Aggressive Reduction in Cholesterol Levels trial.