Mycobacterium leprae

Background

Microbiology

• Slow-growing Gram-positive and acid-fast bacillus

Epidemiology

• About 1 million cases worldwide each year, but is rare in North America
  • Number may be underestimated due to difficulties with reliable diagnosis
• Most commonly occurs in Southeast Asia (especially India) and Brazil
• Decreasing incidence over the past several decades, likely due to short-course multidrug therapy starting in 1982
• Humans are thought to be the main reservoir, but it has been found in animals as well (particularly nine-banded armadillos)
• Transmitted most likely by respiratory droplets, though can also be transmitted by direct contact, transplacentally, through breast milk, and after animal exposure

Risk Factors

• Age, with peaks in adolescence and ≥30 years
• Adult men (compared to adult women)
• Duration of contact with an infected patient, and the burden of bacilli in the patient

Pathophysiology

• The clinical spectrum of disease depends on the host immune response to infection
• A robust Th1 CD4 response causes tuberculoid leprosy, which is paucibacillary and well-controlled
  • Requires interferon-γ
• A Th2 CD4 response causes lepromatous leprosy, which is multibacillary and more progressive

Clinical Manifestations

• Following exposure, about 95% clear it spontaneously
• For those who do not, there is an incubation period of 3-5 years (with wide range) that is usually followed by indeterminate leprosy
  • Single, ill-defined, hypopigmented skin lesion
  • About 75% spontaneously resolve, with the other 25% progressing
• Classic presentation is anaesthetic hypopigmented skin lesion with thickened nerves
• Skin lesions can be: annular, asymmetric macules or plaques with central clearing and elevated borders (in tuberculoid) or symmetric, poorly-demarcated nodules and plaques or diffuse infiltration (lepromatous)
  • Lepromatous can also have xanthoma-likek or dermatofibroma-like lesions, leonine facies, and eyebrow alopecia

Spectrum of Disease

• Clinical spectrum can be classified based on the number of lesions and burden of mycobacteria
  • Paucibacillary (PB) disease has 1 to 5 skin lesions, without bacilli on skin slit smear
  • Multibacillary (MB) disease has more than 5 skin lesions, with or without nerve involvement or bacilli on slit-skin smear (regardless of number of lesions)
• Can also be classified based on general clinical appearance
  • Tuberculoid leprosy (TT) corresponds to paucibacillary
  • Borderline tuberculoid leprosy (BT)
  • Borderline leprosy (BB)
  • Borerdline lepromatous leprosy (BL)
  • Lepromatous leprosy (LL) corresponding to multibacillary disease

Type I Reaction

• A cell-mediated hypersensitivity reaction that can develop in the course of treatment
• Also known as a reversal reaction due to the apparent worsening of the lesion
• Occurs most commonly in the borderline cases and may signal progression to the cell-mediated tuberculoid end of the clinical spectrum

Type 2 Reaction

• A humorally-mediated hypersensitivity reaction that can develop in the course of treatment
• Also known as erythema nodosum leprosum
• Characterized by systemic illness and immune-complex deposition that appears as groups of tender subcutaneous nodules
• May have other signs of vasculitis, including fevers, arthralgias, neuralgia, lymphadenopathy, orchitis, and dactylitis

Physical Examination

Commonly Affected Nerves

Differential Diagnosis

• Hypopigmented patches: vitiligo, pityriasis alba, post-inflammatory hypopigmentation
• Erythematous macules and plaques: psoriasis, tinea corporis, nummular dermatitis, syphilis, mycosis fungoides, sarcoidosis
• Annular plaques: granuloma annulare, tinea corporis, psoriasis
• Nodules: keloid, dermatofibroma, lymphoma, metastasis, sarcoidosis, non-tuberculous mycobacteria, fungal infection
• Leonine facies: Paget disease of bone, mycosis fungoides, polyostatic fibrous dysplasia, amyloidosis, lichen myxedematosus, leishmaniasis, lipoid proteinosis, progressive nodular histiocytosis, mastocytosis
• Reversal reaction: cellulitis, drug eruption, lymphoma, tumid lupus, Sweet syndrome
• Erythema nodosum leprosum: erythema nodosum, sepsis, panniculitis, flare of connective tissue disease
• Neurologic findings: heritable neuropathies, polyneuropathy, entrapment neuropathy, cervicobrachial and scalenus syndromes, syringomyelia, amyloidosis, neurofibroma
  • Leprosy never causes upper motor neuron lesions, and spares proximal muscles as well as deep tendon reflexes and proprioception
  • Sensory findings in leprosy are worse distally, though there may be islands of preserved sensation
  • Leprosy never involves CNS

Diagnosis

• Worldwide, the diagnosis is made based on clinical findings with or without slit-skin smears or biopsy
  • At least one of: loss of sensation in a hypopigmented or reddish skin patch; thickened or enlarged peripheral nerve with loos of sensation and/or muscle weakness; or presence of acid-fast bacilli in slit-skin smear
  • A positive slit-skin smear is diagnostic of multibacillary disease
• Slit-skin smear is made by scraping with a scalpel blade an opening of small slits made in pinched skin
  • The expressed tissue fluid is smeared on a slide and stained for acid-fast bacilli by Fite’s method
  • The pinching makes the skin relatively avascular, to minimize contamination with blood
  • Initial skin smears are usually taken from the routine sites of both earlobes, elbows, and knees, as well as several typical lesions from the patient
• Skin biopsy may be more useful in high resource settings
  • Biopsy should be taken from the lesion edge of the most active margin of the most active lesion
  • Ideally full-thickness biopsy including dermis; can be a punch biopsy
  • Stained with Fite staining to maximize sensitivity

Management

WHO Recommendations

National Hansens's Disease Program (US)

Second-Line Antibiotics

• Clarithromycin
• Minocycline
• Fluoroquinolones: ofloxacin, levofloxacin, or moxifloxacin

Management of Reactions