TWO DECADES OF USING THE COMBINATION OF TETRACYCLINE DERIVATIVES AND NIACINAMIDE AS STEROID-SPARING AGENTS IN THE MANAGEMENT OF PEMPHIGUS: DEFINING A NICHE FOR THESE LOW TOXICITY AGENTS MORGAN MCCARTY, DO, AND DAVID FIVENSON, MD ANN ARBOR, MICHIGAN BS. Vương Thế Bích Thanh
Background: The treatment of pemphigus vulgaris (PV) and pemphigus foliaceous (PF): systemic, topical steroids, immunosuppressive, immunomodulatory agents Twin goals: long-term disease control, minimizing toxicities related to immunosuppression → effective steroid-sparing agents TCN/NAM: a steroid-sparing therapy for bullous pemphigoid. Pemphigus: 1993, Chaffins: reported 11 patients (5 complete responders, 4 partial responders, and 2 nonresponders). 1995, Alpsoy reported 10 patients (2 complete responders, 3 partial responders, and 5 nonresponders)
Objectives: This retrospective review details 20 years of 1 practitioner’s experience using TCN/NAM as steroid sparing agents in the management of pemphigus, determine the effects of TCN/NAM on autoantibody levels during the long-term treatment of pemphigus
Methods : All pemphigus patients in a private medical dermatology office setting, from 1993 to 2013 All newly diagnosed or flaring pemphigus patients who were treated with TCN/NAM after initial oral steroid induction therapy for active pemphigus Excluded: Patients who underwent all other therapies Defined TCN/NAM responder: disease remission, control on minimal therapy, or only transient lesions within 3 months of starting this regimen Side effects related to TCN/NAM therapy Anti-desmoglein 1 (DSG1), anti-desmoglein 3 (DSG3) ELISAs Statistical analysis: correlate the clinical response with antibody levels
Results: 83 patients, 32 excluded: taking a variety of therapeutic agents 51 active disease (43 PV, 7 PF, 1 PE) : oral corticosteroids (1-2 mg/kg/day) with TCN/NAM (tetracycline 500 mg 4 times daily, doxycycline 100 mg twice daily, or minocycline 100 mg twice daily) initiated as soon as active blistering had stopped. Oral corticosteroids: tapered 10% per week over 2 to 3 months duration of clinical response: 1 to 13 years (mean, 3.14 ± 2.97 years), disease duration: 1 to 23 years (mean, 8.63 ± 4.63 years) 46: responded with disease control after 3 months, 3 lost to follow-up
Results: 13 (9 PV+4 PF): completely controlled on TCN/NAM alone 28 (23 PV + 4 PF + 1 PE): partially controlled 5 PV (10%): nonresponders →46 of 51 (90%): disease control on minimal therapy Antidesmoglein titers trended lower in TCN/NAM responders desmoglein 3 approached statistical significance (antiedesmoglein 1,P=0.21; antiedesmoglein 3, P= 0.02)
Discussion:
Tetracyclines: decrease interleukin (IL)-1b, matrix metalloproteinases (matrix metalloproteinase-13) Niacinamide: inhibition of serum phosphodiesterase, increasing cyclic adenosine monophosphate, inhibiting antigen-immunoglobulin E-induced histamine release (ie, mast cell stabilization), inhibition of ILs-1b, -6, and -8, tumor necrosis factor alfa, transforming growth factor beta- 2, macrophage chemotactic protein -> decreased leukocyte chemotaxis and lymphocyte transformation
Conclusion: TCN/NAM may be useful as a steroid-sparing therapy for pemphigus Help avoid /delay the use of stronger immunosuppressive agents and their associated toxicities.
Limitations: retrospective analysis from a single practice lack of serial autoantibody titers limited statistical analyses
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