Leave a message
info@auctorespublishing.com
+1-(302)-520-2644
+1-(302)-520-2644

The use of mycophenolate mofetil in psoriasis: An educational article and expert opinion

  1. Home
  2. Journals
  3. Clinical Research and Clinical Trials
  4. Archives
Submit Guidelines

Research Article | DOI: https://doi.org/10.31579/2693-4779/141

The use of mycophenolate mofetil in psoriasis: An educational article and expert opinion

  • Aamir Al-Mosawi *

Advisor doctor and expert trainer, The National Center of Training and Development Iraqi Ministry of Health, Baghdad, Iraq.

*Corresponding Author: Aamir Al-Mosawi, Advisor doctor and expert trainer, The National Center of Training and Development Iraqi Ministry of Health, Baghdad, Iraq.

Citation: Aamir Al-Mosawi, (2023), The use of mycophenolate mofetil in psoriasis: An educational article and expert opinion, Clinical Research and Clinical Trials, 7(5); DOI:10.31579/2693-4779/141

Copyright: © 2023, Aamir Al-Mosawi. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Received: 27 July 2023 | Accepted: 16 August 2023 | Published: 05 September 2023

Keywords: psoriasis; expert opinion; mycophenolate

Abstract

Background: Patients with mild psoriasis are generally treated with topical medications including corticosteroids, coal tar, anthralin (Dithranol), salicylic acid, vitamin D analogues such as calcipotriol, retinoid such as tazarotene, and calcineurin inhibitors such as pimecrolimus. The most commonly used safe systemic non-biological medications include methotrexate which has been used as early as the 1960s, mycophenolate mofetil which has been used as early as the 1970s, and acitretin which has been used as early as the 1980s. Safe systemic biological medications include infliximab which has been used as early as 2001. 

Patients and methods: The case of a 51-year-old diabetic and hypertensive male who had moderately severe psoriasis with history of arthritic symptoms is described.   

Results: The patient had been treated with several topical medications for years; however, the steroid containing topical therapies have been recently linked with worsening of hyperglycemia. Therefore, topical treatment was replaced with oral methotrexate 5 mg twice weekly. After few weeks of methotrexate treatment, there was slight improvement, and therefore increasing the dose of methotrexate to 7.5 mg twice weekly was suggested by the earlier treating physician, however, the patient was reluctant to increase the dose methotrexate because he has already aware of the possible hepatotoxic effect. When the patient presented to us, he had significant area of his body affected and systemic treatment was considered necessary. The decision was made to add oral mycophenolate with attempt of gradually withdrawing methotrexate. According to the published experiences with the use of mycophenolate monotherapy in psoriasis, a satisfactory response is expected to occur in about 70% or less, and therefore the decision was made add topical calcipotriol 0.005% and give once daily at night. 

Conclusion: The current evidence-based expert opinion suggests that the choice of the treatment of methotrexate resistant psoriasis depends to a large extent on the availability of the medication, and the experience of the treating physician with the available medications. Mycophenolate can be used safely with beneficial effect in severe psoriasis and methotrexate psoriasis.

Introduction

Psoriasis is a chronic scaling skin disorder associated with systemic manifestations especially arthritic manifestations, and it may affect about 2% of people throughout the world. The disease was most probably first described by the Roman encyclopedist, Cornelius Celsus Patients (Figure-1) [1].

Figure-1: Aulus Cornelius Celsus (25 BC-50 AD), a Roman encyclopedist

Patients with mild disease are generally treated with topical medications including corticosteroids, coal tar, anthralin (Dithranol), salicylic acid, vitamin D analogues such as calcipotriol, retinoid such as tazarotene (AGN 190168), and calcineurin inhibitors such as pimecrolimus [2-6]. 

The most commonly used safe systemic non-biological medications, include methotrexate which has been used as early as the 1960s, mycophenolate mofetil which has been used as early as the 1970s, and acitretin, oral retinoid which has been used as early as the 1980s.Safe systemic biological medications include infliximab which has been used as early as 2001[7-12].

Patients and methods

The case of a 51-year-old diabetic and hypertensive male who had moderately severe psoriasis with history of arthritic symptoms is described. 

Results

The patient had been treated with several topical medications for years; however, the steroid containing topical therapies have been recently linked with worsening of hyperglycemia. Therefore, the earlier treating physician stopped topical treatment and started oral methotrexate 5 mg twice weekly. After few weeks of methotrexate treatment, there was slight improvement, and therefore the earlier treating physician suggested increasing the dose of methotrexate to 7.5 mg twice weekly, however, the patient was reluctant to increase the dose methotrexate because he has already aware of the possible hepatotoxic effect. The patient has already noticed that stopping methotrexate is associated with some increase in the severity of the disease.

When the patient presented to us, he had significant area of his body affected and systemic treatment was considered necessary.

Leukocyte count and liver function testes showed normal findings.

As there are many therapeutic options, the choice of the treatment depends on the availability of the medication, and the experience of the treating physician with the chosen medication. 

Because of our extensive experience with mycophenolate in the treatment of a variety of conditions including refractory urticaria, nephrotic syndrome, and systemic lupus erythematosus, the decision was made to add oral mycophenolate 2000 mg five days a week (Not given during the days when methotrexate is taken) with attempt of gradually withdrawing methotrexate.

According to the published experiences with the use of mycophenolate monotherapy in psoriasis, a satisfactory response is expected to occur in about 70% or less, and therefore the decision was made add topical calcipotriol 0,005% and give once daily at night.

Discussion

<!-- /* Font Definitions */ @font-face {font-family:"Cambria Math"; panose-1:2 4 5 3 5 4 6 3 2 4; mso-font-charset:0; mso-generic-font-family:roman; mso-font-pitch:variable; mso-font-signature:-536869121 1107305727 33554432 0 415 0;} @font-face {font-family:Calibri; panose-1:2 15 5 2 2 2 4 3 2 4; mso-font-charset:0; mso-generic-font-family:swiss; mso-font-pitch:variable; mso-font-signature:-469750017 -1073732485 9 0 511 0;} /* Style Definitions */ p.MsoNormal, li.MsoNormal, div.MsoNormal {mso-style-unhide:no; mso-style-qformat:yes; mso-style-parent:""; margin-top:0cm; margin-right:0cm; margin-bottom:8.0pt; margin-left:0cm; line-height:107%; mso-pagination:widow-orphan; font-size:11.0pt; font-family:"Calibri",sans-serif; mso-ascii-font-family:Calibri; mso-ascii-theme-font:minor-latin; mso-fareast-font-family:Calibri; mso-fareast-theme-font:minor-latin; mso-hansi-font-family:Calibri; mso-hansi-theme-font:minor-latin; mso-bidi-font-family:"Times New Roman"; mso-bidi-theme-font:minor-bidi; mso-ansi-language:EN-US; mso-fareast-language:EN-US; mso-bidi-language:AR-SA;} h1 {mso-style-priority:9; mso-style-unhide:no; mso-style-qformat:yes; mso-style-link:"Heading 1 Char"; mso-style-next:Normal; margin-top:12.0pt; margin-right:0cm; margin-bottom:0cm; margin-left:0cm; line-height:107%; mso-pagination:widow-orphan lines-together; page-break-after:avoid; mso-outline-level:1; font-size:16.0pt; font-family:"Calibri Light",sans-serif; mso-ascii-font-family:"Calibri Light"; mso-ascii-theme-font:major-latin; mso-fareast-font-family:"Times New Roman"; mso-fareast-theme-font:major-fareast; mso-hansi-font-family:"Calibri Light"; mso-hansi-theme-font:major-latin; mso-bidi-font-family:"Times New Roman"; mso-bidi-theme-font:major-bidi; color:#2F5496; mso-themecolor:accent1; mso-themeshade:191; mso-font-kerning:0pt; mso-ansi-language:EN-US; mso-fareast-language:EN-US; mso-bidi-language:AR-SA; font-weight:normal;} p {mso-margin-top-alt:auto; margin-right:0cm; mso-margin-bottom-alt:auto; margin-left:0cm; mso-pagination:widow-orphan; font-size:12.0pt; font-family:"Times New Roman",serif; mso-fareast-font-family:"Times New Roman"; mso-ansi-language:EN-US; mso-fareast-language:EN-US; mso-bidi-language:BN-BD;} span.Heading1Char {mso-style-name:"Heading 1 Char"; mso-style-priority:9; mso-style-unhide:no; mso-style-locked:yes; mso-style-link:"Heading 1"; mso-ansi-font-size:16.0pt; mso-bidi-font-size:16.0pt; font-family:"Calibri Light",sans-serif; mso-ascii-font-family:"Calibri Light"; mso-ascii-theme-font:major-latin; mso-fareast-font-family:"Times New Roman"; mso-fareast-theme-font:major-fareast; mso-hansi-font-family:"Calibri Light"; mso-hansi-theme-font:major-latin; mso-bidi-font-family:"Times New Roman"; mso-bidi-theme-font:major-bidi; color:#2F5496; mso-themecolor:accent1; mso-themeshade:191;} span.authors-list-item {mso-style-name:authors-list-item; mso-style-unhide:no;} span.comma {mso-style-name:comma; mso-style-unhide:no;} .MsoChpDefault {mso-style-type:export-only; mso-default-props:yes; font-family:"Calibri",sans-serif; mso-ascii-font-family:Calibri; mso-ascii-theme-font:minor-latin; mso-fareast-font-family:Calibri; mso-fareast-theme-font:minor-latin; mso-hansi-font-family:Calibri; mso-hansi-theme-font:minor-latin; mso-bidi-font-family:"Times New Roman"; mso-bidi-theme-font:minor-bidi; mso-ansi-language:EN-US; mso-fareast-language:EN-US;} .MsoPapDefault {mso-style-type:export-only; margin-bottom:8.0pt; line-height:107%;} @page WordSection1 {size:612.0pt 792.0pt; margin:72.0pt 72.0pt 72.0pt 72.0pt; mso-header-margin:36.0pt; mso-footer-margin:36.0pt; mso-paper-source:0;} div.WordSection1 {page:WordSection1;} -->

Mycophenolic acid was first isolated by Bartolomeo Gosio (Figure-2) from Penicillium brevicompactum in 1896. However, his discovery was forgotten. However, it was rediscovered by Alsberg and O.M. Black from the United States in 1912. Mycophenolate mofetil (Cellcept), a derivative of mycophenolic acid was introduced by Anthony Allison a geneticist from South African and his wife Elsie M Eugui during the early 1970s, and has become an immunosuppressive agent [13].

Figure-2: Bartolomeo Gosio (17 March17, 1863-April 13, 1944), an Italian medical scientist

Everett Linn Jones from the United States (Figure-3) and his research groups were the first to report the use of mycophenolate mofetil in the treatment of psoriasis during the 1970s.They reported the treatment of 29 patients with psoriasis treated with oral mycophenolate mofetil for at least three months. The daily dose of mycophenolate mofetil was increased from 1.6 to 4.8 g depending on occurrence of adverse effects. One patient experienced total clearing of the skin lesions, and 14 patients experienced almost total clearing of the skin lesions, definite improvement was observed in 13 patients, and slight or doubtful improvement was observed in one patient. However, discontinuing treatment was associated with relapses that were observed at a median time of one month (Range: 3-8 weeks). Side effects included nausea, anorexia, and soft or frequent bowel motions or diarrhea. One patient experienced reversible, dose-related leukopenia [9, 10].

Figure-3: Everett Linn Jones from the United States

In 1977, Lynch and Roenigk reported a placebo-controlled study which included 38 patients with psoriasis treated with mycophenolate. The study showed mycophenolic acid was effective in treating psoriasis (P less than .01) [14].

In 1978, Spatz and colleagues reported a study which included 28 patients with psoriasis. The study showed that about 75% of patients treated with mycophenolate experience good to excellent improvement, and toxicity was low. Spatz and colleagues emphasized that mycophenolate can be very useful in treating patients with severe psoriasis [15].

In 1979, Gomez and colleagues reported a placebo-controlled study which included 21 patients with psoriasis. 10 of 11 patients treated with mycophenolate experienced more than 25% reduction in severity while only 2 of 10 patients treated with placebo experience such improvement. 

The placebo group experienced a slight increase in severity, while patients treated with mycophenolate experienced about 50

Conclusion

The current evidence-based expert opinion suggests that the choice of the treatment of methotrexate resistant psoriasis depends to a large extent on the availability of the medication, and the experience of the treating physician with the available medications. Mycophenolate can be used safely with beneficial effect in severe psoriasis and methotrexate psoriasis.

Acknowledgement

The author has the copyrights of the sketches included in this paper.

Conflict of interest

None.

References

  1. Benedek TG. (2013). Psoriasis and psoriatic arthropathy, historical aspects: part I. J Clin Rheumatol 19(4):193-8.
    View at Publisher | View at Google Scholar
  2. Seville RH. (1966). Dithranol paste for psoriasis. Br J Dermatol 78(5):269-72.
    View at Publisher | View at Google Scholar
  3. Scarpa C. (1994). Calcipotriol: clinical trial versus betamethasone dipropionate + salicylic acid. Acta Derm Venereol Suppl (Stockh). 186:47.
    View at Publisher | View at Google Scholar
  4. Esgleyes-Ribot T, Chandraratna RA, Lew-Kaya DA, Sefton J, Duvic M. (1994). Response of psoriasis to a new topical retinoid, AGN 190168. J Am Acad Dermatol 30(4): 581-90.
    View at Publisher | View at Google Scholar
  5. Kumar B, Kumar R, Kaur I. (1997). Coal tar therapy in palmoplantar psoriasis: old wine in an old bottle? Int J Dermatol; 36(4):309-12.
    View at Publisher | View at Google Scholar
  6. Mrowietz U, Graeber M, Bräutigam M, Thurston M, Wagenaar A, Weidinger G, Christophers E. (1998). The novel ascomycin derivative SDZ ASM 981 is effective for psoriasis when used topically under occlusion. Br J Dermatol 139(6):992-6.
    View at Publisher | View at Google Scholar
  7. Van Scott EJ, Auerbach R, Weinstein GD:(1964). Parenteral methotrexate in psoriasis. Arch Dermatol 89: 550- 556.
    View at Publisher | View at Google Scholar
  8. McDonald CJ, Bertino JR. (1969). Parenteral methotrexate in psoriasis. A report on the efficacy and toxicity of long-term intermittent treatment. Arch Dermatol 1 100:655- 668.
    View at Publisher | View at Google Scholar
  9. Jones EL, Epinette WW, Hackney VC, Menendez L, Frost P: Treatment of psoriasis with oral mycophenolic acid (abstract). J Invest Dermatol 1973; 60:246.
    View at Publisher | View at Google Scholar
  10. Jones EL, Epinette WW, Hackney VC, Menendez L, Frost P. (1975). Treatment of psoriasis with oral mycophenolic acid. J Invest Dermatol. 65(6):537-42.
    View at Publisher | View at Google Scholar
  11. Goldfarb MT, Ellis CN, Gupta AK, Tincoff T, Hamilton TA, Voorhees JJ. (1988). Acitretin improves psoriasis in a dose-dependent fashion. J Am Acad Dermatol 18(4 1):655-62.
    View at Publisher | View at Google Scholar
  12. Ogilvie AL, Antoni C, Dechant C, Manger B, Kalden JR, Schuler G, Lüftl M. (2001). Treatment of psoriatic arthritis with antitumour necrosis factor-alpha antibody clears skin lesions of psoriasis resistant to treatment with methotrexate. Br J Dermatol 144(3):587-9.
    View at Publisher | View at Google Scholar
  13. Kitchin JE, Pomeranz MK, Pak G, Washenik K, Shupack JL. (1997). Rediscovering mycophenolic acid: a review of its mechanism, side effects, and potential uses. J Am Acad Dermatol. 37(31):445-9.
    View at Publisher | View at Google Scholar
  14. Lynch WS, Roenigk HH Jr.?(1977). Mycophenolic acid for psoriasis. Arch Dermatol 113(9):1203-8.
    View at Publisher | View at Google Scholar
  15. Spatz S, Rudnicka A, McDonald CJ. (1978). Mycophenolic acid in psoriasis. Br J Dermatol 98(4):429-35
    View at Publisher | View at Google Scholar
  16. Gomez EC, Menendez L, Frost P. (1978). Efficacy of mycophenolic acid for the treatment of psoriasis. J Am Acad Dermatol 1(6):531-7.
    View at Publisher | View at Google Scholar
  17. Geilen CC, Arnold M, Orfanos CE. (2001). Mycophenolate mofetil as a systemic antipsoriatic agent: positive experience in 11 patients. Br J Dermatol .144(3):583-6.
    View at Publisher | View at Google Scholar
  18. Zhou Y, Rosenthal D, Dutz J, Ho V. (2003). Mycophenolate mofetil (CellCept) for psoriasis: a two-center, prospective, open-label clinical trial. J Cutan Med Surg .7(3): 193-7.
    View at Publisher | View at Google Scholar
  19. Herrera J, Ferrebuz A, MacGregor EG, Rodriguez-Iturbe B. (2006). Mycophenolate mofetil treatment improves hypertension in patients with psoriasis and rheumatoid arthritis. J Am Soc Nephrol. 17(12 3):218-25.
    View at Publisher | View at Google Scholar
a