Puva therapy

Author: Prof. Dr. med. Peter Altmeyer

Last updated on: 29.10.2020

Synonym(s)

Balneophotochemotherapy; Photochemotherapy

Definition
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Local or systemic application of methoxsalen (= psoralen; tricyclic furanocoumarin) for photosensitization with subsequent UVA irradiation. Methoxsalen (8-Methoxypsoralen; 8-MOP) or trimethylpsoralen (TMP) are mainly used. These are deposited in the cutaneous DNA and form non-covalent bonds (intercalation). By irradiation with long-wave UV light (UVA, 320-400 nm) at an action maximum at approx. 355 nm, the psoralens enter into a covalent bond with pyrimidine bases (especially thymine).

Effects
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Reduction of allergic late type reactions by reducing the number of Langerhans cells in the epidermis and thus reducing contact sensitization.
Reduction of keratinocyte proliferation.
Reduction of markers of epidermal activity such as keratin 16 or TGF-α.
Reduction of immunologically active proteins expressed by keratinocytes (HLA-DR, ICAM-1, IP-10), which are held responsible for the interaction with T-lymphocytes in psoriasis, for example.
Suppression of epidermal and dermal lymphocyte count and lymphocyte activity (CD3+, CD4+, CD8+, IL-2 receptor+), also in vivo.
Effect on cytokines (TGF-α, IL-2, IL-6, IL-8, TNF-α, IFN gamma) and on molecules which can directly promote hyperproliferation of the epidermis (e.g. EGF, IGF-1, IL1 receptors, see growth factors below).
Inhibition of DNA synthesis, increase in the rate of sister-chromatide exchange and increase in chromosome aberrations.

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Allergology

Pruritus

Frequently occurring symptom that requires very differentiated treatment (polyetiological) in numerous skin...

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Indication
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Possible indications are:

alopecia areata
Eczema: Dermatitis, hypereosinophilic; eczema, atopic (except photoaggravated atopic eczema); eczema, contact allergic (hand and foot eczema); eczema, hyperkeratotic-rhagadiform hand and foot eczema.
Graft versus host disease (acute and chronic forms)
annular granuloma
lichen planus
Mycosis fungoides or cutaneous T-cell lymphoma in stages 1a, 1b and possibly 2a
Papulose, lymphomatoid
Pityriasis lichenoides (acute and chronic form), Pityriasis rubra pilaris
Photodermatoses (hardening with systemic PUVA therapy or PUVA bath therapy) e.g.: reticuloid, actinic; light reaction, persistent; light dermatosis, polymorphic; dermatitis, chronic actinic; light urticaria, Hidroa vacciniformia
protoporphyria, erythropoietic
Prurigo shapes
Psoriasis vulgaris, psoriasis (pustulosa) palmoplantaris
Scleroderma, circumscripts
Scleromyxoedema
urticaria pigmentosa
Vitiligo.

Implementation
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Systemic intake of Methoxsalen: see below PUVA therapy, systemic.
Local application of Methoxsalen: see below PUVA Bath Therapy.

In general (according to E. Hölzle: Guidelines Phototherapy and Photochemotherapy):

First treatment dose 50-70% of the MPD or standard regimen according to skin type (see below the respective treatment types). Continuation of treatment 2-4 times/week.
No erythema and good response: increase the UVA dose by 30% twice a week.
Minimal erythema: no increase in UVA dose.
Persistent asymptomatic erythema: no increase.
Persistent symptomatic erythema (painful with or without edema or blistering): no further treatment until the symptoms subside.
Resumption of treatment: After the symptoms have subsided, reduction of the last dose by 50%, further increases of 10%.

Undesirable effects
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Acute 1st to 2nd degree burns with overdose, itching, nausea. If eye protection is missing, keratitis photoelectrica.
Chronic radiation damage to the skin: The most important long-term side effect of PUVA therapy is spinocellular carcinoma. After about 200-300 treatments, a significant increase in the skin tumour rate (primarily spinocellular carcinomas, hardly any basal cell carcinomas; no malignant melanomas!) by a factor of about 10-12 has been described. Further described are elastosis actinica; lentigines; melanoma, malignant, lentigo-maligna melanoma; basal cell carcinoma; testicular carcinoma in men (gonad protection!), questionable cataract formation (eye protection!).

Contraindication
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Increased risk of carcinoma: history of arsenic, pretreatment with ionising radiation, malignant skin tumours or dysplastic pigment moles, use of immunosuppressive drugs.
Increased photosensitivity: intake of photosensitizing drugs such as: tetracyclines, sulfonamides, diuretics. External use of photosensitizing substances such as tetracyclines, benzoyl peroxide, St. John's wort oil.
Photosensitive dermatoses: Herpes simplex infection, dermatomyositis, lupus erythematosus, photosensitive genodermatoses, photoaggravated endogenous eczema.
Especially in the case of oral PUVA treatment: severe liver and kidney damage (if necessary, consult an internist).
Especially during PUVA bath/shower treatment: cardiovascular problems, open wounds.
Other: Pregnancy, lactation, children under 12 years.

Note(s)
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The UVA initial dose depends on the individual sensitivity to the phototoxic reaction, which is defined by the minimum phototoxic dose ( MPD).
An increased risk of lymphoma in psoriatic patients after PUVA therapy does not seem to exist. On the other hand, the risk is increased in patients who simultaneously received a high cumulative dose of methotrexate.

Literature
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Diederen PV et al (2003) Narrowband UVB and psoralen-UVA in the treatment of early-stage mycosis fungoides: a retrospective study. J Am Acad Dermatol 48: 215-219
Farr PM et al (1984) PUVA treatment of scleromyxoedema. Br J Dermatol 110: 347-350
Friedmann PS (1981) Disappearance of epidermal Langerhans cells during PUVA therapy. Br J Dermatol 105: 219-221
Girbig P et al (1988) Special late effects in PUVA patients. Act Dermatol 15: 28-31
Hölzle E et al (2003) Recommendations for phototherapy and photochemotherapy. SDDG 1: 985-995
Honigsmann H (2001) Phototherapy for psoriasis. Clin Exp Dermatol 26: 343-350
Ibbotson SH et al (2001) The effect of methoxsalen dose on ultraviolet-A-induced erythema. J Invest Dermatol 116: 813-815
Kwok YK et al (2002) Psoralen photochemotherapy (PUVA) is only moderately effective in widespread vitiligo: a 10-year retrospective study. Clin Exp Dermatol 27: 104-110
Stern RS (2006) Lymphoma risk in psoriasis: results of the PUVA follow-up study. Arch Dermatol 142: 1132-1135
Stern RS et al (1990) Genital tumors among men with psoriasis exposed to psoralens and ultraviolet A radiation (PUVA) and ultraviolet B radiation. N Engl J Med 322: 1093-1097
Wolff K (1985) PUVA Pro and Contra. dermatologist 36: 25-33