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Risk-optimized use of Janus kinase inhibitors in Japanese patients with rheumatoid arthritis depends on comorbiditiesNew evidence helps doctors choose safer arthritis treatments for seniors

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Key Takeaway
Consider individual comorbidity profiles and infection risks rather than age alone when selecting Janus kinase inhibitors.

This narrative review evaluates the safety profile and clinical utility of Janus kinase inhibitors (JAKi) for patients with rheumatoid arthritis in Japan, including those who are older or have multiple comorbidities. The authors synthesize evidence to determine how risk should be optimized when selecting JAKi therapies compared to biologic disease-modifying antirheumatic drugs.

The review identifies herpes zoster as the most consistent safety signal associated with JAKi use. In contrast, hospitalized infections were not consistently higher in older patients treated with JAKi than those on biologics. The authors note that evidence regarding major adverse cardiovascular events (MACE), venous thromboembolism (venous thromboembolism), and malignancy remains limited or inconsistent within the Japanese context.

A primary finding is that while older age is an important factor, it is not a sufficient determinant of safety; outcomes are more strongly influenced by glucocorticoid exposure, laboratory abnormalities, and specific comorbidities. The authors acknowledge limitations including heterogeneity in study designs and patient backgrounds, as well as inconsistent data regarding certain serious adverse events.

Clinically, the review supports a risk-optimized approach. Treatment decisions should be individualized based on a patient's specific comorbidity profile, infection risk, and malignancy background rather than age alone. The authors caution that current data do not support routine selection of JAKi based primarily on JAK selectivity.

How this fits prior evidence

This narrative review addresses the safety of Janus kinase inhibitors in Japanese patients with rheumatoid arthritis. It extends prior coverage regarding the reassuring malignancy safety of targeted synthetic DMARDs by highlighting that while herpes zoster is a consistent signal, evidence for MACE and malignancy remains limited or inconsistent in this specific population. The findings suggest that individualized risk-optimization based on comorbidities is key for managing these patients.

Living with rheumatoid arthritis can be challenging, especially as patients get older and manage other health issues. Doctors often have to decide which medications offer the best balance of safety and effectiveness. A recent review of data from Japan helps clarify how to choose these treatments for older adults.

The study looked at Janus kinase inhibitors (JAKi), a type of medication used to manage arthritis. While some feared that age alone would make these drugs risky, the evidence shows that a patient's specific health profile matters much more. Factors like existing infections, heart risks, and how much steroid medicine they use are better indicators of safety than their birth year.

The most consistent safety concern found was herpes zoster, which is the virus that causes shingles. Other serious issues, like heart problems or blood clots, showed inconsistent results in the Japanese data. Because every patient is different, doctors can now move toward a risk-optimized approach. This means they can tailor treatment based on an individual's specific risks rather than making broad assumptions based on age.

What this means for you:
A patient's specific health risks and conditions are better predictors of drug safety than age alone.

Common questions

Is it safe for older patients to take Janus kinase inhibitors?

Age alone is not the only factor in determining if these drugs are safe. While being older is a factor, a patient's specific health issues, such as their risk of infection or heart problems, play a much larger role in deciding if the treatment is right for them.

What are the most common side effects of these medications?

The most consistent safety signal found was herpes zoster (shingles). While other serious issues like hospitalized infections, heart problems, or blood clots were monitored, they did not show a consistently higher risk for patients taking Janus kinase inhibitors compared to other treatments.

How do doctors decide which treatment is best for an older patient?

Doctors use a risk-optimized approach. Instead of looking only at age, they look at the individual's specific health profile, including their history of infections, heart risks, and any history of cancer to choose the safest path forward.

Study Details

Study typeSystematic review
EvidenceLevel 1
PublishedJun 2026
View Original Abstract ↓
BackgroundJanus kinase inhibitors (JAKi) have expanded treatment options for rheumatoid arthritis (RA) by providing rapid and effective oral therapy. However, their optimal use has become increasingly complex after the emergence of safety concerns involving serious infections, herpes zoster (HZ), major adverse cardiovascular events (MACE), venous thromboembolism (VTE), and malignancy. This issue is particularly relevant in Japan, where the RA population is older and has a higher prevalence of comorbidities.ObjectiveTo review the risk-optimized use of JAKi for RA based on Japanese evidence, with particular emphasis on older patients, comorbidity-rich populations, and practical real-world treatment decision-making.Evidence acquisitionWe conducted a literature search of PubMed/MEDLINE and Ichushi-Web to identify Japan-specific studies on JAKi in RA. Randomized trials, long-term extension studies, registry analyses, database studies, postmarketing surveillance reports, and observational studies were reviewed. Because of heterogeneity in design, patient background, and outcome definitions, the evidence was synthesized narratively.ContentJapanese evidence indicates that older age is an important but insufficient determinant of JAKi safety. Across studies, treatment outcomes were more strongly influenced by comorbidities, glucocorticoid exposure, laboratory abnormalities, and other patient-related risk factors. HZ emerged as the most consistent safety signal, supporting the importance of vaccination and early monitoring. By contrast, the risk of hospitalized infection was not consistently higher with JAKi than with biologic disease-modifying antirheumatic drugs in older patients, and Japanese evidence on MACE, VTE, and malignancy remained limited or inconsistent. Real-world studies also supported individualized dose optimization, whereas current data did not support routine within-class selection based primarily on JAK selectivity.ConclusionCurrent Japanese evidence supports a risk-optimized approach to the use of JAKi in RA. Age alone should not determine treatment decisions. Instead, rheumatologists should individualize JAKi selection, dosing, and monitoring according to comorbidity profile, infection and vascular risk, malignancy background, and therapeutic priorities, particularly in increasingly older and multimorbid patients.
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