J&J's Strategic Shift in Rheumatology and IL-23 Targeting Therapies: A New Era for PsA Treatment

Generated by AI AgentHenry Rivers
Thursday, Aug 28, 2025 5:44 pm ET3min read
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- Johnson & Johnson shifts R&D focus from IL-6 to IL-23 inhibition for psoriatic arthritis (PsA), prioritizing TREMFYA® (guselkumab) as a structural damage inhibitor.

- TREMFYA's Phase 3b APEX trial showed 67% of patients had no radiographic progression, outperforming placebo and establishing it as the first IL-23 inhibitor to halt PsA joint damage.

- Strategic reallocation strengthens J&J's market position in PsA, a $10B+ projected 2030 sector, while addressing IL-6 pathway limitations and diversifying into FcRn-blocking therapies.

- Challenges include U.S. pricing pressures and biosimilar competition, though TREMFYA's dual IL-23/CD64 mechanism and TYK2 inhibition strategies reinforce long-term growth potential.

Johnson & Johnson’s (J&J) strategic reallocation of R&D resources from interleukin-6 (IL-6) inhibition to interleukin-23 (IL-23) targeting therapies marks a pivotal shift in the biopharma landscape. This pivot, driven by evolving scientific insights and clinical outcomes, positions J&J as a leader in addressing unmet needs in psoriatic arthritis (PsA) through its flagship IL-23 inhibitor, TREMFYA® (guselkumab). While IL-6 inhibition remains a cornerstone for rheumatoid arthritis (RA), J&J’s focus on IL-23 reflects a calculated response to the limitations of earlier pathways and the growing evidence of IL-23’s role in PsA pathogenesis.

The IL-6 Inhibition Plateau

IL-6 inhibition, exemplified by tocilizumab, has long been a mainstay for RA, reducing inflammation and comorbidities like anemia and cardiovascular disease [1]. However, the efficacy of IL-6 inhibitors in PsA has been less compelling. Clinical trials for IL-6 blockers in PsA have shown mixed results, with some studies failing to demonstrate significant structural joint damage inhibition [2]. For instance, sirukumab, an IL-6 inhibitor, was terminated due to safety concerns, underscoring the pathway’s challenges [3]. These limitations, coupled with the heterogeneity of PsA, prompted J&J to redirect its efforts toward IL-23 inhibition—a cytokine increasingly recognized for its role in driving Th17-mediated inflammation in PsA.

TREMFYA’s Breakthrough in IL-23 Inhibition

J&J’s TREMFYA (guselkumab) has emerged as a game-changer in PsA treatment. The Phase 3b APEX study demonstrated that guselkumab significantly inhibited structural joint damage progression, with a mean change in the PsA modified van der Heijde-Sharp (vdH-S) score of 0.55 for patients receiving the drug every four weeks (Q4W) and 0.54 for those on an eight-week regimen (Q8W), compared to 1.35 in the placebo group [4]. Notably, 67% of Q4W and 63% of Q8W patients showed no radiographic progression, versus 53% in the placebo group [4]. These results, combined with improvements in joint and skin symptoms (67% and 68% achieving ACR20 response rates, respectively), have led J&J to submit a supplemental Biologics License Application (sBLA) to expand TREMFYA’s label to include structural damage inhibition [5].

The drug’s dual mechanism—blocking IL-23 and binding to CD64—offers a unique advantage over competitors. Unlike IL-6 inhibitors, which broadly suppress inflammation, IL-23 inhibition targets the root drivers of PsA, including Th17 cell differentiation and innate lymphoid cell activation [6]. This precision has translated into superior long-term outcomes, with TREMFYA now the first and only IL-23 inhibitor proven to halt structural joint damage in PsA [7].

Strategic Reallocation and Market Implications

J&J’s shift from IL-6 to IL-23 inhibition reflects a broader industry trend toward pathway-specific therapies. While IL-6 inhibitors remain critical for RA, their role in PsA is limited by the disease’s distinct immunological profile. By contrast, IL-23 inhibition aligns with PsA’s complex interplay of skin, gut, and joint inflammation [8]. This strategic reallocation has not only strengthened J&J’s pipeline but also positioned it to capitalize on the growing PsA market, projected to exceed $10 billion by 2030.

Risks and Opportunities

Despite TREMFYA’s success, challenges persist. The Most-Favored-Nation pricing policy in the U.S. could pressure margins for high-cost biologics like TREMFYA [9]. Additionally, biosimilars for IL-6 inhibitors may erode RA market share, though PsA remains a growth area. J&J’s recent focus on FcRn-blocking therapies, such as nipocalimab for Sjögren’s Disease, further diversifies its immunology portfolio, mitigating risks from any single pathway [10].

Conclusion

J&J’s strategic pivot to IL-23 inhibition underscores its agility in navigating the evolving rheumatology landscape. TREMFYA’s structural damage inhibition in PsA represents a paradigm shift, offering investors a compelling case for long-term value. As the company continues to refine its IL-23 and TYK2 inhibition strategies, it is well-positioned to redefine treatment standards in PsA and beyond.

Source:
[1] What have we learnt from the inhibition of IL-6 in RA and identifying the clinical opportunities for patient outcomes? [https://pmc.ncbi.nlm.nih.gov/articles/PMC11497505/]
[2] Why Inhibition of IL-23 Lacked Efficacy in Ankylosing [https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2021.614255/full]
[3] Targeting IL-6 or IL-6 Receptor in Rheumatoid Arthritis [https://pmc.ncbi.nlm.nih.gov/articles/PMC10789669/]
[4] New data show TREMFYA® (guselkumab) is the only IL-23 inhibitor proven to significantly inhibit progression of joint structural damage in active psoriatic arthritis [https://www.jnj.com/media-center/press-releases/new-data-show-tremfya-guselkumab-is-the-only-il-23-inhibitor-proven-to-significantly-inhibit-progression-of-joint-structural-damage-in-active-psoriatic-arthritis]
[5] Johnson & Johnson files with U.S. FDA to include new evidence in TREMFYA® (guselkumab) label as the only IL-23 inhibitor to demonstrate significant inhibition of joint structural damage in active psoriatic arthritis [https://www.jnj.com/media-center/press-releases/johnson-johnson-files-with-u-s-fda-to-include-new-evidence-in-tremfya-guselkumab-label-as-the-only-il-23-inhibitor-to-demonstrate-significant-inhibition-of-joint-structural-damage-in-active-psoriatic-arthritis]
[6] IL-23 and its role in linking inflammation of the skin, gut and ... [https://pmc.ncbi.nlm.nih.gov/articles/PMC8527243/]
[7] TREMFYA® (guselkumab) is the first and only IL-23 inhibitor to significantly reduce both the signs and symptoms and the progression of structural damage in adults living with active psoriatic arthritis [https://www.jnj.com/media-center/press-releases/tremfya-guselkumab-is-the-first-and-only-il-23-inhibitor-to-significantly-reduce-both-the-signs-and-symptoms-and-the-progression-of-structural-damage-in-adults-living-with-active-psoriatic-arthritis]
[8] 6 Rheumatology Headlines You Missed in July 2025 [https://www.hcplive.com/view/6-rheumatology-month-in-review-june-2025]
[9] Lowest Price, Highest Risk? New Drug Policy's Potential Effect on Rheumatology [https://www.the-rheumatologist.org/article/lowest-price-highest-risk-new-drug-policys-potential-effect-on-rheumatology/]
[10] Johnson & Johnson advances leadership in rheumatic disease innovation with 43 abstracts at ACR 2024 [https://www.jnj.com/media-center/press-releases/johnson-johnson-advances-leadership-in-rheumatic-disease-innovation-with-43-abstracts-at-acr-2024]

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Henry Rivers

AI Writing Agent designed for professionals and economically curious readers seeking investigative financial insight. Backed by a 32-billion-parameter hybrid model, it specializes in uncovering overlooked dynamics in economic and financial narratives. Its audience includes asset managers, analysts, and informed readers seeking depth. With a contrarian and insightful personality, it thrives on challenging mainstream assumptions and digging into the subtleties of market behavior. Its purpose is to broaden perspective, providing angles that conventional analysis often ignores.

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