Kissing Lesions (Cutaneous Leishmaniasis)
Overview
Cutaneous leishmaniasis (CL) is a skin infection caused by protozoan parasites of the genus Leishmania that are transmitted to humans through the bite of infected sandâflies. âKissing lesionsâ describe a characteristic presentation in which two or more adjacent lesions appear as mirrorâimage nodules that touch or âkissâ each other, often on exposed body surfaces such as the face, arms, or legs.
CL affects roughly 0.7â1.2 million new people each year worldwide, with the highest burden in the Middle East, Central and South America, the Indian subâcontinent, and the Mediterranean basin [1][2]. While the disease can affect anyone exposed to infected sandâflies, certain groupsârural agricultural workers, military personnel, and people living in poorâhousing conditionsâare disproportionately affected.
Symptoms
The clinical picture varies according to parasite species, host immunity, and lesion location. The typical course includes:
- Incubation period: 1â12 weeks after the sandâfly bite.
- Papule: A small, raised, erythematous bump (5â10âŻmm) that may be painless or mildly itchy.
- Plaque: The papule enlarges into a flat or slightly raised plaque, often with a central area of necrosis.
- Ulceration: Central ulcer with a raised, indurated border; the base may be granulating, serous, or hemorrhagic.
- Kissing lesions: Two ulcers develop sideâbyâside, appearing to âkissâ each other; common on the lips, eyelids, and limbs.
- Satellite lesions: Smaller nodules around a larger ulcer.
- Scarring: After healing, lesions often leave atrophic or hypertrophic scars, sometimes with pigment changes.
- Systemic signs (rare): Lowâgrade fever, malaise, or lymphadenopathy, mainly in diffuse or mucocutaneous forms.
Patients may also report burning, tenderness, or secondary bacterial infection, especially when lesions are scratched.
Causes and Risk Factors
What causes kissing lesions?
Cutaneous leishmaniasis is caused by infection with one of >20 Leishmania species. The most common species that produce typical âkissingâ lesions are L. major, L. tropica, and L. mexicana. The life cycle involves:
- Infected female sandâfly (Phlebotomine) takes a blood meal and inoculates metacyclic promastigotes into the dermis.
- Parasites are phagocytosed by macrophages and transform into amastigotes.
- Amastigotes multiply intracellularly, causing local inflammation and tissue destruction that manifest as lesions.
Who is at higher risk?
- Geographic exposure: Residence or travel to endemic regions (e.g., Afghanistan, Brazil, Iran, Syria, Colombia, Saudi Arabia).
- Occupational exposure: Farmers, construction workers, soldiers, and outdoor laborers who work at dusk or night when sandâflies are most active.
- Poor housing: Mud walls, cracks, and lack of window screens increase indoor sandâfly exposure.
- Immunosuppression: HIV infection, organ transplantation, or corticosteroid therapy can worsen disease severity.
- Age: Children often develop more prominent lesions due to thinner skin.
- Gender: Some endemic areas report higher rates in males because of occupational exposure.
Diagnosis
Accurate diagnosis combines clinical assessment with laboratory confirmation.
Clinical Evaluation
- History of travel/exposure to endemic areas.
- Physical exam noting lesion morphology (look specifically for âkissingâ lesions).
Laboratory Tests
- Microscopy (Giemsa stain): Skinâscraping or biopsy material shows intracellular amastigotes (âLeishmanâDonovan bodiesâ). Sensitivity 50â70âŻ%.
- Culture: NNN (NovyâMcNealâNicolle) or Schneiderâs medium grows promastigotes; takes 1â4 weeks.
- Polymerase Chain Reaction (PCR): Highly sensitive (â„95âŻ%) and speciesâspecific; increasingly the reference standard [3].
- Histopathology: Biopsy shows granulomatous inflammation with macrophages containing amastigotes; helps differentiate from other ulcerative skin diseases.
- Serology: Generally not useful for localized CL but can aid in mucocutaneous or diffuse forms.
Differential Diagnosis
Consider other ulcerative skin conditions: bacterial cellulitis, atypical mycobacterial infection, fungal infections, pyoderma gangrenosum, basal cell carcinoma, and cutaneous tuberculosis.
Treatment Options
Treatment goals are lesion clearance, prevention of scarring, and avoidance of mucosal spread. Choice depends on parasite species, lesion number/size, location, patient comorbidities, and drug availability.
Systemic Antiparasitic Medications
- Sodium stibogluconate (SSG) or meglumine antimoniate: Pentavalent antimonials are firstâline in many regions; 20âŻmg/kg daily for 20â30 days. Monitoring for cardiotoxicity and hepatic dysfunction is essential [4].
- Amphotericin B (liposomal formulation): Effective for antimonyâresistant disease; 3âŻmg/kg on days 1â5, 10, 17, 24, and 31. Requires renal monitoring.
- Miltefosine: Oral agent (2.5âŻmg/kg/day divided BID for 28 days). FDAâapproved for leishmaniasis; teratogenicâcontraindicated in pregnancy.
- Paromomycin (topical or intralesional): 15âŻ% cream BID for 4â6 weeks, or intralesional injection (0.5â1âŻmL per lesion) weekly for 4â6 weeks; useful for single or few lesions.
Local Therapies (for limited lesions)
- Thermotherapy: Controlled heating of the lesion to 50â55âŻÂ°C for 30âŻseconds; cure rates 70â90âŻ% for L. major and L. tropica.
- Cryotherapy: Liquid nitrogen freezeâthaw cycles; may be combined with intralesional antimonials.
- Electroâdesiccation & Curettage: Mechanical removal of lesion tissue; best for small, wellâcircumscribed nodules.
Adjunctive Measures
- Analgesics (acetaminophen or ibuprofen) for pain.
- Topical antibiotics if secondary bacterial infection develops.
- Silicone gel sheets or pressure therapy after healing to reduce hypertrophic scarring.
Special Considerations
Pregnant women, children, and immunocompromised patients require tailored regimens (e.g., lowerâdose antimonials, close monitoring, or use of liposomal amphotericin B).
Living with Kissing Lesions (Cutaneous Leishmaniasis)
Daily Management Tips
- Wound care: Clean lesions gently with saline; avoid harsh scrubbing.
- Dressings: Use nonâadhesive sterile gauze; change daily or if soiled.
- Protect from sunlight: UV exposure can worsen hyperpigmentation; apply broadâspectrum SPFâŻ30+ sunscreen after the lesion starts to heal.
- Nutrition: Maintain a balanced diet rich in protein, zinc, and vitamin C to support immune function and wound healing.
- Avoid scratching: Trim fingernails and keep lesions covered to prevent secondary bacterial infection.
- Psychosocial support: Visible facial lesions can cause anxiety; counseling or support groups can help.
- Followâup: Attend scheduled appointments for treatment response and scar management.
Prevention
- Vector control: Use insecticideâtreated bed nets, indoor residual spraying, and environmental management (eliminate sandâfly breeding sites such as organic waste piles).
- Personal protection: Wear long sleeves, trousers, and closed shoes during duskâtoâdawn hours; apply repellents containing DEET (â„30âŻ%) or picaridin.
- Housing improvements: Seal cracks in walls, install fineâmesh screens on windows and doors.
- Travel precautions: Seek preâtravel counseling for endemic regions; consider prophylactic measures if staying for extended periods.
- Vaccination research: Experimental vaccines are under investigation but not yet available for public use.
Complications
If untreated or inadequately treated, CL can lead to:
- Persistent or enlarging ulcers: May become secondarily infected with bacteria (e.g., Staphylococcus aureus, Streptococcus pyogenes).
- Scarring: Disfiguring atrophic or hypertrophic scars, especially on the face.
- Mucocutaneous leishmaniasis: Spread to mucosal surfaces (nasal, oral, pharyngeal) causing destructive lesions, common with L. braziliensis complex.
- Diffuse cutaneous leishmaniasis: Nonâulcerating nodules that spread widely; associated with immunosuppression.
- Psychological impact: Stigma, low selfâesteem, and depression.
When to Seek Emergency Care
- Rapidly spreading redness, swelling, or pain around a lesion indicating possible cellulitis or necrotizing infection.
- FeverâŻâ„âŻ38.5âŻÂ°C (101.3âŻÂ°F) accompanied by chills.
- Severe pain unrelieved by overâtheâcounter analgesics.
- Signs of systemic involvement: difficulty breathing, persistent vomiting, or confusion.
- Lesion involvement of the eyelids, nose, or oral mucosa causing functional impairment (e.g., vision loss, severe bleeding).
References:
- World Health Organization. Leishmaniasis. WHO Fact Sheet, 2022.
- Mayo Clinic. Cutaneous leishmaniasis: Symptoms and causes. Updated 2023.
- Schön T, et al. Molecular diagnosis of cutaneous leishmaniasis by PCR. Clin Microbiol Rev. 2021;34(2):e00123â20.
- National Institute of Allergy and Infectious Diseases. Treatment of leishmaniasis. NIH Guidelines, 2022.