Sudan Journal of Medical Sciences
Volume 14, Issue no. 1, DOI 10.18502/sjms.v14i1.4375
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Research Article

Treatment of Extensive Plaque Psoriasis and
Psoriatic Arthropathy Using Methotrexate in
a Patient with High Serum Alkaline
Phosphatase
Suad HH1, Muna Mohammed El Amin2, Gad Allah Modawe3, and
Osman Elbasheer4

1Department of Dermatology, Omdurman Islamic University, Omdurman, Sudan
2Department of Community Medicine, Omdurman Islamic university, Omdurman, Sudan
3Department of Biochemistry, Omdurman Islamic University, Omdurman, Sudan
4Khartoum Dermatology Teaching Hospital, Khartoum State, Sudan

Abstract
Background: Psoriasis is an autoimmune inflammatory, chronic, and relapsing disease
of the skin, which can also present with severe joint inflammation and deformity. There
are many treatment options, but the severe forms of psoriasis are treated successfully
with cytotoxic and biologic therapies. Methotrexate being cheap and available in Sudan
is considered a good option for patients with severe and extensive forms of psoriasis.
One of the main drawbacks is hepatotoxicity. The aim of this report is to share an
experience of treating the patient with oral methotrexate in the presence of a relative
contraindication to this therapy.
Method: We present a 60-year-old female with extensive skin psoriasis and psoriatic
arthropathy. Investigations showed high serum alkaline phosphatase and low serum
albumen. Other liver enzymes, CBC, ultrasound abdomen were all unremarkable.
Patient was admitted and a weekly dose of methotrexate was given in addition to
topical preparation and supportive treatment; three months later, patient improved and
was moved to topical therapy. A check of serum alkaline phosphatase and albumen
every week was done.
Results: The patient was successfully and safely treated with methotrexate. Serum
alkaline phosphatase was normal within the second month treatment, and serum
albumen was normal after only one month of treatment.
Conclusion: High serum alkaline phosphatase is considered a relative contraindication
to the use of methotrexate, high level can be found in bone diseases. Serum albumen
can be low in dermatologic diseases with excessive shedding of scales and can be
corrected with protein formulas and high protein diets.
Recommendations: Methotrexate is recommended for the treatment of severe morbid
forms of psoriasis. The biologic therapy for severe forms of psoriasis is now available
and can be a good alternative for the treatment of severe forms of psoriasis in good
centers and for patients who can afford and in patients with absolute contraindications
to methotrexate therapy.

Keywords: psoriasis, psoriatic arthropathy, alkaline phosphatase, methotrexate

How to cite this article: Suad HH, Muna Mohammed El Amin, Gad Allah Modawe, and Osman Elbasheer (2019) “Treatment of Extensive Plaque
Psoriasis and Psoriatic Arthropathy Using Methotrexate in a Patient with High Serum Alkaline Phosphatase,” Sudan Journal of Medical Sciences,
vol. 14, issue no. 1, pages 1–8. DOI 10.18502/sjms.v14i1.4375

Page 1

Received 21 January 2019

Accepted 26 March 2019

Published 31 March 2019

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Suad HH et al. This article

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Prof. Mohammad A. M. Ibnouf

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1. Introduction

Psoriasis is a particular autoimmune systemic inflammatory disease of great interest. It
has a chronic, relapsing, and remitting course that has devastating impact on a person’s
health-related quality of life (HRQL) [1].

Psoriasis is a common health problem with an estimated worldwide prevalence of
2–3%, with great regional and ethnic variations. Caucasians predominate [2].

Few studies have reported on the incidence of psoriasis in the Middle East, including
two small single-center studies conducted in 2004 that found the incidence of psoriasis
to be 3.4%, in the south-western and eastern Saudi Arabia (3).

Similar to all autoimmune diseases, the pathophysiology of psoriasis is so compli-
cated, not yet fully understood, and expresses a mixture of genetic, environmental and
behavioral influences. While, clinically, the signs and symptoms appear to be caused
by hyper proliferation and inflammation of epidermal cells. In psoriasis, an immunologic
response involving T-lymphocytes and cytokines alters the epidermal skin cell cycle to
result in the formation of the psoriatic plaques, the whole mark of the disease [4].

Since the mid-1950s, methotrexate has become the gold standard by which other
systemic psoriasis medications are measured (5).

In 1972, the Food and Drug Administration (FDA) approved methotrexate for the
treatment of psoriasis and provided a formal basis for its use. Guidelines are published
since this approval to standardize the use of methotrexate. These guidelines addressed
indications, contraindications, pretreatment evaluation, monitoring of therapy, dosages,
adverse reactions, and overdose. The original guidelines endorsed liver biopsy as the
gold standard for detecting liver damage and introduced a histological classification
standard for grading liver biopsy specimens. Since their original publication in 1972, the
guidelines have continued to evolve over the years and have undergone four revisions
[6, 7].

The latest set was published in 1998 where liver biopsies were replaced by blood
tests for liver fibrosis, serum aminoterminal propeptide of type III procollagen (PIIIPN),
based on results of small studies [8].

Methotrexate is a relatively safe medication as a serious damage to the liver undis-
putedly occurs in less than 1% or even less than 0.1% of the patients. The burden for
patients might not outweigh the potential damage [9].

Efforts to treat severe psoriasis continues to increase; in 1974, a survey revealed that
52% of dermatologists used methotrexate to treat psoriasis, this increased in 1987 when
another survey showed that the number of dermatologists who used methotrexate had

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increased slightly to 58%. In 2001, millions of prescriptions were written for methotrexate,
of which approximately 11% were for psoriasis (9).

Administered either as monotherapy or in combination with the other schemes,
methotrexate exerts its effects by acting as both immunomodulatory and anti-metabolite
agent due to the downregulation of T-cell-mediated pro-inflammatory markers and
inhibition growth of keratinocytes and decrease in the endothelial expression of ICAM-1
and E-selectin (10).

Clinical data from trials suggest that 24% and 100% of psoriasis patients achieved
PASI-75 at week 12 at MTX dosage of 7.5 and 15 mg, respectively. However, we found
that 73% and 40% of patients reached PASI-75 at week 12 in group B and A, respectively
(11).

During 1985, Lanes et al. had followed 30 patients with psoriasis and other nonma-
lignant diseases with liver biopsies done before treatment with low-dose methotrexate,
15 mg/week, and then at one- to two-year intervals as long as they continued the
methotrexate. All patients were symptomatically improved on this regimen. The 15
patients who had normal liver biopsies at the start of the study had normal biopsies after
methotrexate, 15 others had minor hepatic histological abnormalities before treatment,
11 had fatty infiltration, 10 showed no significant change after treatment, while 1 had
increased fat and portal fibrosis on a fourth liver biopsy done seven years after MTX was
begun. This last patient, a former alcohol abuser, continued methotrexate and showed
no further worsening at 8 years. The remaining four had portal fibrosis before treatment.
One patient had less fibrosis after methotrexate, two patients slightly more fibrosis, and
one a marked increase in portal fibrosis. No patient developed cirrhosis or clinical liver
disease. These results suggest that in the absence of alcohol consumption, low-dose
weekly methotrexate treatment rarely causes clinically significant liver damage.

Similar results for hepatotoxicity associated with low-dose, long-term methotrexate
treatment of rheumatoid arthritis was shown by Szanto et al. in 1987.

Relative contraindication for methotrexate therapy include kidney failure, gastric ulcer,
hypoalbuminemia, elevated liver enzymes, active infectious diseases, treatment with
immunosuppressant, interactions with other drugs, hyperlipidemia, folic-acid deficiency,
alcohol abuse, obesity, diabetes, active or past history of hepatitis, lack of patient
compliance, and old age. While there are some other conditions that are considered
absolute contraindications for treatment with methotrexate (12).

Case report: A 60-year old female, married and residing in Gezeira state has a

known case of chronic plaque psoriasis since 20 years, with remissions and relapses,

emollients and some preparations being used according to dermatologist prescription.

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In the last presentation, the patient had an extensive involvement of her skin affecting

the extensors of limbs, face, trunk more marked over the lower parts and scalp. The

condition was associated with severe bilateral hip joint pain and finger deformities, so

severe that the patient had to use a wheel chair.

Pt was otherwise normal, no complains related to other systems, no abdominal

pain, no chest pain, no palpitations or headache. No past history of schistosomiasis,

hematuria, malèna, jaundice, or liver disease. No previous hospital admission. Pt not

known diabetic or hypertensive. No family history of psoriasis or other skin disease. No

history of alcohol consumption. Not on chronic medication, apart from the preparations

for psoriasis. Patient is a house wife; her husband is an employee in a company with

a low income, she is postmenopausal, with two daughters and two sons.

O l E: Patient was uncomfortable, pushed on a wheel chair. Not pale or jaundiced.

Normal pulse and BP. No palpable lymph nodes. Lower limbs: pitting edema present

bilaterally.

Examination of the chest and heart revealed no abnormality.

Abdomen showed no tenderness, no organomegaly. Liver was of normal size.

Skin: Lesions were located over the extensors of both upper and lower limbs, face

and trunk involvement was more extensive on the lower half with no specific pattern

of distribution in the form of well-demarcated papules and plaques covered with easily

detached white silvery scales. The skin between the lesions is erythematous and

tender.

Scalp: All covered with easily detached scales with well-demarcated psoriatic

corona.

Palms and soles show hyperkeratosis. Mucous membranes were normal.

Joints: Painful interphalangeal joints with finger deformities. Bilateral painful tender

hips.

Investigations: Urine and stool analysis showed no abnormality. CBC showed slightly

raised WBC. RBCs, Hb, and platelets were all normal.

Liver function tests: Slight increase of alkaline phosphatase and Low serum albumen,

other liver enzymes were all normal.

Renal function tests and electrolytes were normal.

Rheumatoid factor –ve.

US abdomen: No organomegaly, liver is of normal size and texture, and no evidence

of chronic liver disease.

X-Ray hips and X-Ray hands: inflammatory changes consistent with psoriatic arthritis.

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CXR: clear.

ECG: Normal.

2. Plan of Management

Admission, treatment with General measures included emollients, protein formulas, high
protein diet, tonics, and systemic antibiotics. Specific measures included methotrexate
tabs 15 mg/week divided in three doses 12 hours apart with 5 mg folic acid tabs, skin
preparation included 5% salicylic acid and 4% coal tar in 100 g Vaseline once a day.
Coal tar shampoo for the scalp every other day.

Follow-up included daily assessment of the clinical state, mainly for the regression of
psoriatic plaques, erythema, scales, and lower limb edema. Eye examination for jaundice
is important, hip and finger examination for normal non-restricted joint movement should
all be performed. Follow-up by investigations included weekly measurement of liver
function tests with enzymes and CBC.

3. Outcome

After the second week, the condition improved in terms of edema, joint pain, and skin
condition. In the third and fourth weeks, much improvement was seen and the patient
could stand with support. The second month, the patient could walk with support,
and so static improvement was noticed. At the end of the third month, the patient
was discharged in good condition and could walk unsupported with marked clinical
improvement of the skin condition on topical treatment with coal tar in Vaseline and
divobet (divonex + betamethasone) cream. Follow-up by investigations showed weekly
reduction of alkaline phosphatase level and was normal by the fifth week. Hemoglobin
level was low in the third month for which ferrous sulphate was prescribed. Serum
albumin was corrected by diet and protein formula, and it was normal after one month.

On discharge, liver function test was normal including alkaline phosphatase. Patient
was discharged in good condition with respect to the clinical and laboratory status.

4. Discussion

Psoriasis is an autoimmune chronic inflammatory skin disease with remissions and
relapses; it can affect joints causing psoriatic arthritis and can be so severe leading to
erythroderma.

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The treatment of the localized forms can usually improve with topical agents, but
severe forms like extensive plaque psoriasis, pustular psoriasis, psoriatic arthritis, and
erythrodermic psoriasis need systemic treatment as well. Psoriatic arthritis occurs in
30% of patients. It can result in permanent joint damage, methotrexate is the most
commonly prescribed medication together with NSAIDS.

Methotrexate is a relatively safe cytotoxic antimetabolite drug that has been approved
by the FDA for the treatment of severe variants of psoriasis since 1972 [6, 7]. Serious
damage due to methotrexate occurs in less than 1% or even less than 0.1% of patients [9].
It is effective in the treatment of severe forms of psoriasis, it acts as immunomodulatory
and antimetabolite due to the down regulation of T-cell-mediated pro-inflammatory
markers (10).

Studies done showed that in the absence of alcohol consumption, a weekly low dose
of methotrexate rarely causes clinically significant liver damage. Guidelines for the use
of methotrexate had been studied and clearly stated [6, 7].

The treatment of the reported case was considered challenging because of the
need to a systemic medication, the options are methotrexate, cyclosporine and biologic
therapy; the last two are very expensive in Sudan and the patient couldn’t afford it; the
former is cheap but the patient has an elevated alkaline phosphatase and low serum
albumin which are considered relative contraindications for its use (12). In one study,
portal fibrosis was encountered after seven years of use of methotrexate in a patient
with psoriasis. Follow-up of liver damage was done through biopsies which were then
replaced by the blood tests in 1998 by FDA (8).

Alkaline phosphatase is found in various tissues in the body, highest concentrations
being found in the liver and bones; elevated levels can indicate tissue damage mainly
bone or liver.

Hypo albuminemia can be found in patients with scaly skin diseases where excessive
shedding of scales takes place.

The American Academy of Dermatology suggests the following investigations before
starting treatment with methotrexate: CBC, S. Creatinine, blood urea nitrogen, and liver
function tests with enzymes. Depending on all of the aforementioned facts, a decision
for managing the patient with methotrexate was made. The plan was: Admission, base
line investigations, weekly oral methotrexate, topical antipsoriasis treatment, systemic
antibiotics for UTI, supportive therapy and tonics, clinical follow-up, and through inves-
tigations such as liver function tests and CBC.

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Baseline investigations done were normal apart from minor UTI, elevated serum
alkaline phosphatase, low serum albumin, inflammatory changes of hand and hip joints
indicating psoriatic arthritis.

The patient was well managed with systemic therapy using weekly doses of
methotrexate in addition to topical therapy using salicylic acid and coal tar preparations.

The treatment of this patient was really challenging. Methotrexate is a cheap med-
ication but it is hepatotoxic. This patient has high serum alkaline phosphatase and
low serum albumen, on the other hand, the biologic therapy is highly expensive and
unaffordable by the patient.

5. Conclusion

In the absence of liver disease and alcohol consumption excluded by history, exam-
ination and investigations, high serum alkaline phosphatase is considered a relative
contraindication to methotrexate therapy that can be given successfully and safely to
patients with severe forms of psoriasis under close supervision in the ward.

6. Recommendation

Methotrexate is recommended for the treatment of severe morbid forms of psoriasis.

For those who can afford or in good centers the other option is the biologic therapy
or cyclosporine mainly in patients with absolute contraindications to methotrexate.

References

[1] Rapp, S. R., Feldman, S. R., Exum, M. L., et al. (1999). Psoriasis causes as much
disability as other major medical diseases. Journal of the American Academy of
Dermatology, vol. 41, p. 401e7

[2] National Institute for Health and Clinical Excellence. (2008). Infliximab for
the treatment of psoriasis. Retrieved from: http://www.nice.org.UK/TA134> (last
accessed July 25, 2008).

[3] Alakloby, O. M. (2005). Pattern of skin disease in eastern Saudi Arabia. Saudi Medical
Journal, vol. 26, p. 1610.

[4] National Institute for Health and Clinical Excellence. (2008). Adalimumab for the
treatment of psoriasis. Retrieved from: http://www.nice.org.UK/TA146 (last accessed

DOI 10.18502/sjms.v14i1.4375 Page 7

http://www.nice.org.UK/TA134
http://www.nice.org.UK/TA146


Sudan Journal of Medical Sciences Suad HH et al

August 30, 2008).

[5] Roenigk, H. H., Auerbach, R., Maibach, H. I., et al. (1998). Methotrexate in psoriasis:
consensus conference. Journal of the American Academy of Dermatology, vol. 38,
pp. 478–485.

[6] Roenigk, H. H., Maibach, H. I., and Weinstein, G. P. (1973). Methotrexate therapy for
psoriasis, guideline revisions. Archives of Dermatology, vol. 108, p. 35.

[7] Roenigk, H. H., Auerbach, R., Maibach, H. I., et al. (1982). Methotrexate guidelines–
revised. Journal of the American Academy of Dermatology, vol. 6, pp. 145–155.

[8] Martyn-Simmons, C. L., Rosenberg, W. M. C., Cross, R., et al. (2014). Validity of
noninvasive markers of methotrexate-induced hepatotoxicity: a retrospective cohort.
Dermatology, vol. 171, no. 2, pp. 267–273. Retrieved from: https://doi.org/10.1111/bjd.
12782

[9] Peckham, P. E., Weinstein, G. D., and McCullough, J. L. (1987). The treatment of severe
psoriasis, a national survey. Archives of Dermatology, vol. 123, pp. 1303–1307.

[10] Dahlman-Ghozlan, K., Ortonne JP, Heilborn J, et al. Altered tissue expression pattern
of cell adhesion molecules, ICAM-1, E-selectin and VCAM-1, in bullous pemphigoid
during methotrexate therapy. Exp Dermatol 2004;13:65e9.

[11] Montaudi,_E. H., Sbidian, E., Paul, C., et al. (2011). Methotrexate in psoriasis: a
systematic review of treatment modalities, incidence, risk factors and monitoring of
liver toxicity. Journal of the European Academy of Dermatology and Venereology,
vol. 25, p. 12.

[12] Retrieved from: https://www.researchgate.net.

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	Introduction
	Plan of Management
	Outcome
	Discussion
	Conclusion
	Recommendation
	References