BAD Guidelines for the management of onychomycosis

Published On 2018-03-01 13:32 GMT | Update On 2023-06-17 06:47 GMT

British Association of Dermatologists have released its Guidelines for the management of onychomycosis.They have been published in British Journal of Dermatology.Onychomycosis is among the most common nail disorders in adults. The management of onychomycosis requires the correct mycological identification where possible, assessing disease susceptibility and risk factors and deciding what therapy options are most suitable for the clinical form of onychomycosis and aetiological agent.

Definition of onychomycosis

The term tinea unguium is used to describe dermatophyte infections of the fingernails or toenails. Onychomycosis is a less specific term used to describe fungal disease of the nails. The condition is worldwide in distribution. In addition to dermatophytes, it can be caused by a number of other moulds and by Candida species

Aetiology

Risk factors for onychomycosis include:
- increasing age
- peripheral vascular disease
- trauma and hyperhidrosis

Fungal nail disease is more prevalent in:
- men
- individuals with other nail problems such as psoriasis
- people with immunosuppressive conditions, such as diabetes mellitus or HIV infection
- those taking immunosuppressive medications

Rationale for treating onychomycosis

Onychomycosis can have a significant impact on the quality of life of patients. Problems associated with onychomycosis include discomfort, difficulty in wearing footwear and walking, cosmetic embarrassment and lowered self-esteem

Classification/clinical manifestations

Onychomycosis is a fungal infection caused by various pathogens, which can adopt any of several clinical patterns. The five main clinical patterns are:

Distal and lateral subungual onychomycosis (DLSO)

Most common presentation of dermatophyte nail infection. Toenails are more commonly affected than fingernails. The fungus invades the nail and nail bed by penetrating the distal or lateral margins. The affected nail becomes thickened and discoloured, with a varying degree of onycholysis (separation of the nail plate from the nail bed), although the nail plate is not initially affected. The infection may be confined to one side of the nail or spread to involve the whole of the nail bed. In time the nail plate becomes friable and may break up

The most common causative organism is T. rubrum. As DLSO has a similar clinical presentation whether caused by dermatophytes or nondermatophytes, it is important to obtain a nail sample for mycological examination so that the causative organism can be identified

Superficial white onychomycosis

Infection usually begins at the superficial layer of the nail plate and spreads to the deeper layers. Crumbling white lesions appear on the nail surface, particularly the toenails. These gradually spread until the entire nail plate is involved

Proximal subungual onychomycosis

Least common presentation of dermatophyte nail infection in the general population, it is common in people with AIDS. Infection often spreads rapidly from the proximal margin and upper surface of the nail to produce gross white discoloration of the plate without obvious thickening

Endonyx onychomycosis

Instead of invading the nail bed through the nail plate margin, the fungus immediately penetrates the nail plate keratin. The nail plate is discoloured white in the absence of onycholysis and subungual hyperkeratosis. The most common causative organisms are T. soudanense and T. violaceum

Total dystrophic onychomycosis (TDO)

Any of the above varieties of onychomycosis may eventually progress to TDO, where the nail plate is almost completely destroyed. Primary TDO is rare and is usually caused by Candidaspecies, typically affecting immunocompromised patients

Diagnosis

The clinical signs of tinea unguium are often difficult to distinguish from those of a number of other infectious causes of nail damage, such as Candida, mould or bacterial infection. Unlike dermatophytosis, candidosis of the nails usually begins in the proximal nail plate, and nail fold infection (paronychia) is also present. Bacterial infection, particularly when due to Pseudomonas aeruginosa, tends to result in green or black discoloration of the nails. Sometimes bacterial infection can coexist with fungal infection and may require treatment in its own right

Other less common dystrophic nail conditions mimicking onychomycosis are Darier disease and lichen planus, and ichthyotic conditions such as keratosis, ichthyosis and deafness syndrome. Often yellow nail syndrome is falsely identified as a fungal infection. Light green-yellowish pigmentation of the nail plate, hardness and elevated longitudinal curvature are the key clinical characteristics of this nail disease

Repetitive trauma to the nail plate can also result in the abnormal appearance of nails. The nail bed will appear normal if the symptoms are caused by trauma rather than onychomycosis, with a characteristic pattern of intact longitudinal epidermal ridges stretching to the lunula

Essential investigations and their interpretation

The clinical characteristics of dystrophic nails must alert the clinician to the possibility of onychomycosis. Laboratory confirmation of a clinical diagnosis of tinea unguium should be obtained before starting treatment. This is important for several reasons: to eliminate non-fungal dermatological conditions from the diagnosis; to detect mixed infections; and to diagnose patients with less responsive forms of onychomycosis, such as toenail infections due to T. rubrum. Good nail specimens are difficult to obtain but are crucial for maximising laboratory diagnosis

Material should be taken from any discoloured, dystrophic or brittle parts of the nail. The affected nail should be cut as far back as possible through the entire thickness and should include any crumbly material. Nail drills, scalpels and nail elevators may be helpful but must be sterilised between patients. When there is superficial involvement (as in SWO) nail scrapings may be taken with a curette. If associated skin lesions are present, samples from these are likely to be infected with the same organism, and are more likely to give a positive culture.

Traditionally, laboratory detection and identification of dermatophytes consists of culture and microscopy, which yields results within approximately 2–6 weeks

Treatments

Asymptomatic onychomycosis (especially in elderly people) may not require drug therapy

Tables 1 and 2 summarise the drug therapies recommended in this guideline. Please see the full guideline at for full details of the evidence www.bad.org.uk/shared/get-file.ashx?id=2125&itemtype=document

Summary of drug therapies in adults

Systemics
Itraconazole: first line of treatment for dermatophyte onychomycosis	200 mg per day for 12 weeks continuously, or alternatively as ‘pulse therapy’ at a dose of 400 mg per day for 1 week per month. Two pulses are recommended for fingernails and three pulses for toenails It is optimally absorbed with food and an acidic pH Monitoring hepatic function tests is recommended in patients with pre-existing deranged results, in those receiving continuous therapy for more than a month, and with concomitant use of hepatotoxic drugs
Terbinafine: first line of treatment for dermatophyte onychomycosis, and generally preferred over itraconazole	250 mg per day for 6 weeks in fingernail and 12–16 weeks in toenail infection Baseline liver function tests and a complete full blood count are recommended in adult patients with a history of hepatotoxicity or haematological abnormalities
Fluconazole: may be a useful alternative in patients unable to tolerate terbinafine or itraconazole	150–450 mg per week for 3 months in fingernail infections and for at least 6 months in toenail infections Perform baseline liver function tests and full blood count. Monitor liver function tests in high-dose or prolonged therapy and in those at risk because of concomitant hepatotoxic drug use
Griseofulvin: lower efficacy and higher relapse rates compared with terbinafine and itraconazole	500–1000 mg per day given for 6–9 months in fingernail infection and 12–18 months in toenail infection. It should be taken with fatty food to increase absorption
Combination treatment: recommended if response to topical monotherapy is likely to be poor
Topicals
Amorolfine: useful for superficial and distal onychomycosis	5% lacquer applied once or twice a week for 6–12 months
Ciclopirox: useful for superficial and distal onychomycosis and for patients in whom systemic therapy is contraindicated	8% lacquer applied once daily for up to 48 weeks
Tioconazole: useful for superficial and distal onychomycosis	28% solution applied twice daily for 6–12 months

Summary of drug therapies in children (age 1–12 years)

Treatment in children	Suggested method of use and monitoring
Itraconazole: first line of treatment for dermatophyte onychomycosis	‘Pulse therapy’ 5 mg kg^-1 per day for 1 week per month. Two pulses are recommended for fingernails and three pulses for toenails. It is optimally absorbed with food and an acidic pH Monitoring hepatic function tests is recommended in patients with pre-existing deranged results, in those receiving continuous therapy for more than a month, and with concomitant use of hepatotoxic drugs
Terbinafine: first line of treatment for dermatophyte onychomycosis and generally preferred over itraconazole	62.5 mg per day if weight is <20 kg, 125 mg per day for 20–40 kg weight, and 250 mg per day for > 40 kg, for 6 weeks in fingernail and 12 weeks in toenail infection Baseline liver function tests and a complete full blood count are recommended in paediatric patients as it is unlicensed for use in children
Fluconazole: consider as second line if itraconazole and terbinafine contraindicated or not tolerated	3–6 mg kg^-1 once a week for 12–16 weeks for fingernail and 18–26 weeks for toenail infection Perform baseline liver function tests and full blood count. Monitor liver function tests in high-dose or prolonged therapy and in those at risk because of concomitant hepatotoxic drug use
Griseofulvin: consider as second line if itraconazole and terbinafine contraindicated or not tolerated	10 mg kg^-1 per day for age groups of 1 month and above (maximum 500 mg) It should be taken with fatty food to increase absorption

Treatment failure or relapse?

Onychomycosis has often been associated with high recurrence rates (40–70%), and many patients have a long history of disease recurrence. The term ‘recurrence’ suggests both relapse and reinfection. In treatment relapse, infection is not completely cured and returns. This implies treatment failure

Fungal-free nails are the goal of antifungal therapy in onychomycosis. Because of the slow growth pattern of the toenails, up to 18 months is required for the nail plate to grow out fully. Therapeutic success of antifungal therapy of onychomycosis depends on the newly grown-out nail plate being fungus free

The major risk factors for recurrence include family history, coexisting ancillary clinical conditions (diabetes, arterial and vascular diseases, Down syndrome, Raynaud syndrome), immune suppression and acquired or inherent immunodeficiency. Other previously implicated prognostic factors are coexisting bacterial/viral nail infections, erroneous diagnosis, poor compliance, antifungal resistance and poor choice of antifungal therapy. Furthermore, the role of disease-causing fungi is also critical. Generally, onychomycosis caused by nondermatophytic moulds does not respond to oral antifungal therapy, and current effective management options are limited

Prevention

Strategies include:
- wearing protective footwear to avoid re-exposure
- application of an absorbent powder, and antifungal powders in shoes and on the feet
- wearing cotton, absorbent socks
- discarding all ‘old and mouldy’ footwear
- keeping nails as short as possible and to avoid sharing toenail clippers with family members and friends
- treating all infected family members at the same time to avoid reinfection
- wearing comfortable, well-fitting shoes and to avoid trauma to the nail
- advise patient (if relevant) to be aware of the risk of infection in nail salons—visit salons that employ a sterile technique

Summary of the management of onychomycosis

Onychomycosis is among the most common nail disorders in adults. The management of onychomycosis requires the correct mycological identification where possible, assessing disease susceptibility and risk factors and deciding what therapy options are most suitable for the clinical form of onychomycosis and aetiological agent. Some patients will require monitoring, particularly high-risk patients, and at the end of the recommended course of treatment they should be reassessed for mycological cure (which is defined as negative mycological analysis and a normal nail)

Criteria for referral

Refer to dermatology when:
- oral antifungal treatment is required for a child under 18 years
- diagnosis is uncertain
- treatment is unsuccessful
- person is immunocompromised

Refer to podiatry if nails are traumatised by the person’s footwear, or deformed toenails traumatise adjacent toes

Please see full guideline for further information on:

Candidal onychomycosis

Mould (nondermatophytic) infection of nails

Nondermatophyte moulds

Molecular diagnostics

Histology

Treatment of paediatric onychomycosis

Combination treatment

Onychomycosis in special groups

Surgery, lights, and lasers

For further reference log on to :

www.bad.org.uk/shared/get-file.ashx?id=2125&itemtype=document

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