Psoriasis is a systemic inflammatory disease increasingly recognized as a human model to study inflammatory atherogenesis. While the link between psoriasis and cardiovascular disease is well documented, the mechanistic pathway that connects skin inflammation to systemic inflammation and ultimately to atherosclerosis and cardiovascular events has not been fully elucidated. This study is the first to demonstrate, using robust mediation analysis, that systemic inflammation—measured through GlycA levels—partially mediates the association between psoriasis severity and cardiovascular outcomes.
The interplay between psoriasis and cardiovascular disease has been a topic of intense research and growing clinical concern over the past decade. While observational studies and registry data have consistently shown an increased risk of cardiovascular disease and cardiovascular mortality among patients with moderate to severe psoriasis, the biological mechanisms underlying this association have remained elusive. One prevailing hypothesis is that inflammatory signals originating in psoriatic skin enter the circulation, fueling systemic inflammation that contributes to the development and progression of atherosclerosis.
In this well-conducted study, Svedbom et al. leverage two complementary cohorts to tackle this long-standing question. The Psoriasis Atherosclerosis and Cardiometabolic Disease Initiative (PACI) in the United States assessed subclinical coronary atherosclerosis (non-calcified coronary burden). At the same time, the Stockholm Psoriasis Cohort (SPC) in Sweden followed incident psoriasis cases for cardiovascular events. In both cohorts, higher PASI scores were significantly associated with elevated levels of GlycA, a stable biomarker of systemic inflammation.
The authors used mediation models to assess whether systemic inflammation explained the association between psoriasis severity and cardiovascular disease. Their findings are striking: GlycA mediated approximately 17% of the association with subclinical coronary plaque burden and 37% of the association with clinical cardiovascular events. In the SPC cohort, the association between PASI and cardiovascular events became statistically nonsignificant after adjusting for GlycA, reinforcing the mediating role of systemic inflammation.
This work adds biological plausibility to what clinicians observe daily: patients with more severe psoriasis exhibit greater systemic inflammatory burden, which may increase their cardiovascular risk. It also reinforces the potential of GlycA as a translational biomarker that could bridge dermatology and cardiology.
While the findings are compelling, several questions remain. First, the mediation proportion suggests that systemic inflammation is only part of the story; what other mechanisms are at play? Metabolic dysregulation, insulin resistance, endothelial dysfunction, and treatment effects may all contribute. Recent Mendelian randomization studies suggest that metabolic syndrome and related cardiometabolic alterations may predispose to psoriasis, rather than the reverse. Similarly, genetic liability to cardiovascular disease, particularly coronary artery disease and stroke, has been associated with increased risk of psoriasis, but not vice versa. These findings challenge the notion of a unidirectional, skin-driven model of systemic inflammation. Instead, they underscore the possibility that shared genetic pathways and underlying metabolic dysfunction may simultaneously predispose individuals to both psoriasis and atherosclerosis. Secondly, while GlycA appears promising as a research and possibly clinical tool, its availability and integration into clinical practice are still limited.
Importantly, these findings support the rationale for aggressive management of psoriasis to control skin symptoms and mitigate cardiovascular risk. Whether biologic therapies targeting IL-17, IL-23, or TNF can reduce CV outcomes by attenuating systemic inflammation remains a critical research question. While some evidence suggests a potential benefit, the data remain limited and largely indirect. Prospective trials designed with cardiovascular endpoints, or at least long-term real-world follow-up in registries, are needed to validate this hypothesis.
This study elegantly links skin disease severity to cardiovascular outcomes through systemic inflammation. It underscores the importance of viewing psoriasis as a systemic disease and strengthens the case for a multidisciplinary, comorbidity-conscious approach to patient care. As we continue to refine our understanding of immune-mediated diseases, this work is a timely and significant contribution to the field.
Linking Psoriasis Severity to Cardiovascular Risk: The Role of Systemic Inflammation
Tiago Torres, MD, PhD
Centro Hospitalar Universitário de Santo António, University of Porto
Porto, Portugal
IPC Councilor
PUBLICATION
Skin Inflammation, Systemic Inflammation, and Cardiovascular Disease in Psoriasis. Svedbom A, Mallbris L, González-Cantero Á, et al. JAMA Dermatol. 2025;161(1):81-86. doi:10.1001/jamadermatol.2024.4433
Why This Article Was Chosen
Psoriasis is a systemic inflammatory disease increasingly recognized as a human model to study inflammatory atherogenesis. While the link between psoriasis and cardiovascular disease is well documented, the mechanistic pathway that connects skin inflammation to systemic inflammation and ultimately to atherosclerosis and cardiovascular events has not been fully elucidated. This study is the first to demonstrate, using robust mediation analysis, that systemic inflammation—measured through GlycA levels—partially mediates the association between psoriasis severity and cardiovascular outcomes.
Commentary
The interplay between psoriasis and cardiovascular disease has been a topic of intense research and growing clinical concern over the past decade. While observational studies and registry data have consistently shown an increased risk of cardiovascular disease and cardiovascular mortality among patients with moderate to severe psoriasis, the biological mechanisms underlying this association have remained elusive. One prevailing hypothesis is that inflammatory signals originating in psoriatic skin enter the circulation, fueling systemic inflammation that contributes to the development and progression of atherosclerosis.
In this well-conducted study, Svedbom et al. leverage two complementary cohorts to tackle this long-standing question. The Psoriasis Atherosclerosis and Cardiometabolic Disease Initiative (PACI) in the United States assessed subclinical coronary atherosclerosis (non-calcified coronary burden). At the same time, the Stockholm Psoriasis Cohort (SPC) in Sweden followed incident psoriasis cases for cardiovascular events. In both cohorts, higher PASI scores were significantly associated with elevated levels of GlycA, a stable biomarker of systemic inflammation.
The authors used mediation models to assess whether systemic inflammation explained the association between psoriasis severity and cardiovascular disease. Their findings are striking: GlycA mediated approximately 17% of the association with subclinical coronary plaque burden and 37% of the association with clinical cardiovascular events. In the SPC cohort, the association between PASI and cardiovascular events became statistically nonsignificant after adjusting for GlycA, reinforcing the mediating role of systemic inflammation.
This work adds biological plausibility to what clinicians observe daily: patients with more severe psoriasis exhibit greater systemic inflammatory burden, which may increase their cardiovascular risk. It also reinforces the potential of GlycA as a translational biomarker that could bridge dermatology and cardiology.
While the findings are compelling, several questions remain. First, the mediation proportion suggests that systemic inflammation is only part of the story; what other mechanisms are at play? Metabolic dysregulation, insulin resistance, endothelial dysfunction, and treatment effects may all contribute. Recent Mendelian randomization studies suggest that metabolic syndrome and related cardiometabolic alterations may predispose to psoriasis, rather than the reverse. Similarly, genetic liability to cardiovascular disease, particularly coronary artery disease and stroke, has been associated with increased risk of psoriasis, but not vice versa. These findings challenge the notion of a unidirectional, skin-driven model of systemic inflammation. Instead, they underscore the possibility that shared genetic pathways and underlying metabolic dysfunction may simultaneously predispose individuals to both psoriasis and atherosclerosis. Secondly, while GlycA appears promising as a research and possibly clinical tool, its availability and integration into clinical practice are still limited.
Importantly, these findings support the rationale for aggressive management of psoriasis to control skin symptoms and mitigate cardiovascular risk. Whether biologic therapies targeting IL-17, IL-23, or TNF can reduce CV outcomes by attenuating systemic inflammation remains a critical research question. While some evidence suggests a potential benefit, the data remain limited and largely indirect. Prospective trials designed with cardiovascular endpoints, or at least long-term real-world follow-up in registries, are needed to validate this hypothesis.
This study elegantly links skin disease severity to cardiovascular outcomes through systemic inflammation. It underscores the importance of viewing psoriasis as a systemic disease and strengthens the case for a multidisciplinary, comorbidity-conscious approach to patient care. As we continue to refine our understanding of immune-mediated diseases, this work is a timely and significant contribution to the field.
Categories
Recent Posts
IPC Symposium at the 2026 Society for Investigative Dermatology (SID) Annual Meeting: Disease Interception, Treatment Response, and Immune Escape in Psoriasis
Approaching Challenging Patient Interactions with Empathy
Next Generation of Leaders: 2025 IPC Fellows Transition to Jr. Councilors
Also Read
IPC Symposium at the 2026 Society for Investigative Dermatology (SID) Annual Meeting: Disease Interception, Treatment Response, and Immune Escape in Psoriasis
Read summaries from the IPC symposium at the 2026 Society for Investigative Dermatology (SID) Annual Meeting covering disease modification, immune pathways, therapeutic escape, and psoriasis treatment response.
Highlights from the 2026 American Academy of Dermatology (AAD) Annual Meeting: Diagnostic Complexity, Therapeutic Advances, and Emerging Research
What were the key takeaways from the 2026 AAD Annual Meeting? IPC shares updates on diagnostic challenges, psoriasis therapies, and late-breaking research from leading experts.
First-Line Biologics in Psoriasis: Evidence from the BADBIR Cohort Study
In this IPC commentary, Matias Maskin examines evidence from the BADBIR registry demonstrating that first-line biologic therapy in moderate to severe psoriasis leads to faster skin clearance, improved quality of life, and a lower risk of comorbidities. The analysis challenges traditional step-up approaches and supports earlier, patient-centered treatment strategies.
Subscribe to the IPC Newsletter