6.1.5 Palmoplantar Keratoderma

Grading & Level of Importance: C

Review:

2026

W. Burgdorf, Munich; C. Ellis, A. Salam, J. McGrath, London
Revised by RM Pujol, Barcelona

Overview:

ICD-11
Synonyms
Epidemiology
Definition
Aetiology & Pathogenesis
Signs & Symptoms
Localisation
Classification
Laboratory & other workups
Dermatopathology
Course
Complications
Diagnosis
Differential Diagnosis
Prevention & Therapy
Special

ICD-11

ED55

Synonyms

Keratosis palmoplantaris.

Epidemiology

Includes genetic as well as acquired forms. Uncommon disorders. Autosomal dominant (1:100 000) and autosomal recessive disorders.

Definition

Persistent thickening of the epidermis of palms and soles.

Aetiology & Pathogenesis

Hereditary palmo-plantar keratodermas (PPK) include a high number of genodermatoses with different prognoses with multiple associated cutaneous and extracutaneous features.

Many different genes have been identified in diffuse PPK secondary to keratin mutations (epidermolytic and non-epidermolytic) in an autosomal dominant and recessive pattern of inheritance. Many different clinical variants with multiple implicated genes in focal, striated complex and syndromic hereditary PPKs.

In acquired PPKs, a spectrum of disorders of different etiology may be involved: occupational, irritative, contact allergies, keratoderma climatericum, chemicals, drugs, systemic diseases, malignancies, infectious disorders, inflammatory dermatoses, lymphomas, paraneoplastic etc.

Hereditary palmo-plantar keratodermas (PPK) include a high number of genodermatoses with different prognoses with multiple associated cutaneous and extracutaneous features.

Many different genes identified in diffuse PPK secondary to keratin mutations (epidermolytic and non- epidermolytic) in autosomal dominant and recessive pattern of inheritance. Many different clinical variants with multiple implicated genes in focal, striated, complex and syndromic hereditary PPK (some examples):

Diffuse PPK secondary to KRT1/KRT9 mutations: epidermolytic PPK and non-epidermolytic PPK. Autosomal dominant.
Diffuse PPK secondary to SLURP1 mutations: mal de Meleda. Autosomal recessive.
Diffuse sclerosing palmo-plantar keratoderma (sclerotylosis).
Focal PPK due to KRT6c and KRT16 mutations.
Striate PPK due to Desmoglein 1 and desmoplakin mutations.
Punctate PPK due to AAGAB and COL14A1 mutations.
Complex PPK due to LOR mutations (Vohwinkel syndrome): ichthyosis, PPK, pseudoainhum and mutilations.
Complex PPK due to TRPV3/MBTP2 mutations (Olmsted syndrome): periorificial keratotic plaques, pseudoainhum, hair and nail abnormalities.
PPK with deafness (due to GJB2 mutations, due to MMTS mutations).
PPK with periodontitis (Papillon-Lefèvre syndrome: CTSC mutations).
PPK with arrhythmogenic right/left ventricular cardiomyopathy and woolly hair (Naxos disease/ Carvajal disease): JUP/DSP mutations.

Acquired PPK include a spectrum of disorders of different etiology:

Keratoderma climatericum (women of menopausal age).
Chemicals (arsenic, chloracnegens).
Drugs: Tegafur, bleomycin, hydroxyurea, lithium, verapamil, mepacrine.
Systemic disease (thyroidal disorders, lymphedema).
Malignancies (lymphomas, paraneoplastic).
Infectious disorders (syphilis, tinea, scabies, tuberculosis).
Dermatoses (occupational, irritative, psoriasis, atopic dermatitis, pityriasis rubra pilaris, contact allergies, chronic hand eczema).

Signs & Symptoms

Onset usually in infancy, symmetrical, palms and soles thickened, yellow and fissured with diffuse or focal symmetrical lesions, often hyperhidrosis. Some variants may worsen by age. Association with other ectodermal defects possible.

Acquired PPK may also be focal, diffuse or punctate.

Localisation

Palms and soles. In some cases may extend to the dorsal surfaces of the hands and feet, wrists and Achille’s tendons. Different disorders may present associated hyperkeratotic cutaneous or mucosal lesions, often involving the extensor surfaces of the extremities (knees, elbows), hair, nail and teeth abnormalities.

Classification

Depending on aetiology: Hereditary or acquired PPK

1.1 Hereditary PPK

Diffuse or focal hyperkeratosis, with or without associated findings, exact classification based on molecular genetic identification of mutations. Hereditary PPK can be divided into:

- Non-syndromic isolated PPK: Predominant or unique palmo-plantar involvement

- Complex PPK: Non-syndromic PPK with additional distinctive cutaneous and adnexal manifestations

- Syndromic PPK: PPK associated with specific extracutaneous manifestations

PPK associated with sensorineural deafness
PPK associated with prominent mucosal involvement
PPK associated with cardiomyopathy and woolly hair
PPK associated with other systemic signs

1.2. Acquired PPK

Multiple etiologies: Inflammatory (psoriasis, eczema), systemic diseases, chemicals, drugs, hormonal changes, malignancy, idiopathic.

2. Classification according the observed clinical patterns:

- Diffuse PPK: Generalized epidermal thickening involving the entire palmo-plantar surfaces.

- Focal PPK: Multiple callosities (soles)

- Striate PPK: Linear hyperkeratotic bands in correspondence with the underlying tendons

- Punctate PPK: Multiple papular lesions with epidermal thickening (with a central pit or spiny projection)

Laboratory & other workups

No abnormalities are usually detected. For certain forms in 1.1. molecular profiling has to be done, and for 1.2 individual workup necessary depending on the underlying disease.

Dermatopathology

Non-epidermolytic PPK: Acanthosis, hypergranulosis, hyperkeratosis, orthokeratosis.

Epidermolytic PPK variants: Perinuclear vacuolization, granular degeneration of keratinocytes, large, irregular keratohyaline granules. Subcorneal intaepidermal cleavage.

In acquired PPK the histopathological features are non-specific: hyperkeratosis with orthokeratosis or parakeratosis and different amount of inflammation.

Course

Chronic.

Chronic. Persistent. In some variants of acquired PPK the detection and resolution of the underlying cause may lead to clinical improvement and/or resolution.

Complications

Secondary fungal infection. In syndromic PPK the associated features (cardiomyopathy) may have prognostic implications. Psychosocial problems.

Secondary fungal infection. Psychosocial problems. In some rare variants, sclerotic bands develop around the fingers (pseudoainhum) and automutilation may occur. In syndromic PPK the associated features (i.e., cardiomyopathy) may have prognostic implications.

Diagnosis

Clinical history and features combined with histopathological findings. Positive family history and onset in infancy or childhood may be helpful to distinguish between hereditary and acquired PPK. The clinical pattern (diffuse, striate/focal or punctate) along the presence with other cutaneous or extracutaneous manifestations may also be helpful. In some cases, the genetic study may confirm the diagnosis. In acquired PPK a systematic search for an underlying cause is mandatory.

Differential Diagnosis

The different acquired etiologies that may lead to PPK. Other causes of palmoplantar keratoses: Hand dermatitis (hyperkeratotic, fissured), Psoriasis and hyperkeratotic lesions in secondary syphilis, cutaneous T-cell lymphoma (especially Sézary syndrome), dyskeratosis folicularis (Darier).

Prevention & Therapy

Topical keratolytics: salicylic acid (5-10%), urea, lactic acid, vitamin A acid, abrasive soaps, mechanical removal. Customized footwear.

Systemic: low dose retinoids (acitretin) or 9-cis retinoic acid.

In the acquired variants of PPK: To identify (if possible) and treat the underlying etiology.

Special

None.