Psoriasis adverse events and associated medications as reported in the US Food and Drug Administration’s Adverse Event Reporting System from 2016 to 2021

“…In this respect, the BBs can flare the preexisting PsD in one hand, and induce the de novo PsD in naïve individuals on the other hand. For instance, metoprolol, as a β1 selective blocker-which is one of the widely prescribed BBs in the U.S.-there are 97 reports highlighting that Ps is being the most cutaneous adverse events following metoprolol administration based on US Food and Drug Administration (FDA)'s adverse event reporting system 80 . Beyond the exuberant pre-inflammatory responses, the modification of intracellular calcium (Ca 2+ ) levels, keratinocyte proliferation, and granulocyte function by targeting cyclic adenosine monophosphate (cAMP) pathways are indicated as the underlying mechanisms involved in the BBs-induced psoriasis at the cellular level 81 .…”

“…80, df= 3, I 2 = 90.85). Moreover, the risk of PsD incident in the intervention group is 57% higher than the control group [pooled RR =1.57, 95% CI (1.89-1.95), z-value = 8.07, p-value < 0.001].…”

Causes of Autoimmune Psoriasis and Associated Cardiovascular Disease: Roles of Human Endogenous Retroviruses and Antihypertensive Drugs—A Systematic Review and Meta-analysis

“…In this respect, the BBs can flare the preexisting PsD in one hand, and induce the de novo PsD in naïve individuals on the other hand. For instance, metoprolol, as a β1 selective blocker-which is one of the widely prescribed BBs in the U.S.-there are 97 reports highlighting that Ps is being the most cutaneous adverse events following metoprolol administration based on US Food and Drug Administration (FDA)'s adverse event reporting system 80 . Beyond the exuberant pre-inflammatory responses, the modification of intracellular calcium (Ca 2+ ) levels, keratinocyte proliferation, and granulocyte function by targeting cyclic adenosine monophosphate (cAMP) pathways are indicated as the underlying mechanisms involved in the BBs-induced psoriasis at the cellular level 81 .…”

“…80, df= 3, I 2 = 90.85). Moreover, the risk of PsD incident in the intervention group is 57% higher than the control group [pooled RR =1.57, 95% CI (1.89-1.95), z-value = 8.07, p-value < 0.001].…”

Causes of Autoimmune Psoriasis and Associated Cardiovascular Disease: Roles of Human Endogenous Retroviruses and Antihypertensive Drugs—A Systematic Review and Meta-analysis

“…Because of the discrepancy between the low rates of adverse events in psoriatic patients on systemic glucocorticosteroids and their wide use in this patient population, some argue against the limitation of these agents in psoriasis [ 10 , 12 , 13 ]. Interestingly, a report from the US Food and Drug Administration for the period 2016–2021 determines prednisone as the most common drug related to psoriasis as an adverse event of drug therapy [ 14 ]. Systemic glucocorticosteroids have the potential to exacerbate plaque psoriasis and induce severe forms of the disease but these drugs are indispensable in treating certain comorbidities of psoriasis patients.…”

Drug-related psoriasis

Response to comment on the article entitled “Risk of rebound psoriasis flare from systemic corticosteroid use in patients with psoriasis: A retrospective cohort study”