Mycobacterium leprae: Difference between revisions
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Mycobacterium leprae
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== |
==Background== |
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=== |
===Microbiology=== |
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* Slow-growing [[Stain::Gram-positive]] and Stain::acid-fast]] [[Cellular shape::bacillus]] |
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*Slow-growing [[Stain::Gram-positive]] and [[Stain::acid-fast]] [[Shape::bacillus]] |
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=== 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 |
|||
=== |
===Epidemiology=== |
||
* 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 |
|||
*About 1 million cases worldwide each year, but is rare in North America |
|||
=== Pathophysiology === |
|||
**Number may be underestimated due to difficulties with reliable diagnosis |
|||
* The clinical spectrum of disease depends on the host immune response to infection |
|||
*Most commonly occurs in Southeast Asia (especially India) and Brazil |
|||
* A robust Th1 CD4 response causes tuberculoid leprosy, which is paucibacillary and well-controlled |
|||
*Decreasing incidence over the past several decades, likely due to short-course multidrug therapy starting in 1982 |
|||
** Requires interferon-γ |
|||
*Humans are thought to be the main reservoir, but it has been found in animals as well (particularly nine-banded armadillos) |
|||
* A Th2 CD4 response causes lepromatous leprosy, which is multibacillary and more progressive |
|||
*Transmitted most likely by respiratory droplets, though can also be transmitted by direct contact, transplacentally, through breast milk, and after animal exposure |
|||
===Risk Factors=== |
|||
== 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 |
|||
*Age, with peaks in adolescence and ≥30 years |
|||
=== Spectrum of disease === |
|||
*Adult men (compared to adult women) |
|||
* Clinical spectrum can be classified based on the number of lesions and burden of mycobacteria |
|||
*Duration of contact with an infected patient, and the burden of bacilli in the patient |
|||
** '''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 |
|||
=== |
===Pathophysiology=== |
||
* 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 |
|||
*The clinical spectrum of disease depends on the host immune response to infection |
|||
=== Type 2 reaction === |
|||
*A robust Th1 CD4 response causes tuberculoid leprosy, which is paucibacillary and well-controlled |
|||
* A humorally-mediated hypersensitivity reaction that can develop in the course of treatment |
|||
**Requires interferon-γ |
|||
* Also known as '''erythema nodosum leprosum''' |
|||
*A Th2 CD4 response causes lepromatous leprosy, which is multibacillary and more progressive |
|||
* 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 |
|||
==Clinical Manifestations== |
|||
=== Physical examination === |
|||
==== Commonly affected nerves ==== |
|||
*Following exposure, about 95% clear it spontaneously |
|||
*For those who do not, there is an incubation period of [[Usual incubation period::3-5 years]] (with [[Incubation period range::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==== |
|||
{| class="wikitable" |
{| class="wikitable" |
||
! |
!Trunk!!Palpation!!Sensation!!Movement!!Deformity |
||
|- |
|- |
||
| |
|Ulnar nerve |
||
| |
|Just superior to medial epicondyle |
||
| |
|Fifth digit and ulnar aspect of hand |
||
| |
|Fifth digit abduction |
||
| |
|Claw deformity of little and ring fingers |
||
|- |
|- |
||
| |
|Median nerve |
||
| |
|Palmar wrist just medial to palmaris longus |
||
| |
|Lateral three fingers and palm |
||
| |
|Thumb abduction |
||
| |
|Claw deformity of first through third digits |
||
|} |
|} |
||
== |
== Differential Diagnosis == |
||
=== WHO recommendations === |
|||
* '''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=== |
|||
{| class="wikitable" |
{| class="wikitable" |
||
! |
!Disease!!Treatment |
||
|- |
|- |
||
| |
|Paucibacillary||6 months of [[Is treated by::rifampin]], [[Is treated by::dapsone]], and [[Is treated by::clofazimine]] |
||
|- |
|- |
||
| |
|Multibacillary||12 months of [[Is treated by::rifampin]], [[Is treated by::dapsone]], and [[Is treated by::clofazimine]] |
||
|- |
|- |
||
| |
|Rifampin resistance||6 months of at least two second-line drugs (below) with [[clofazimine]], followed by 18 months of one second-line drug with [[clofazimine]] |
||
|- |
|- |
||
| |
|Quinolone resistance||As for rifampin resistance, but without a fluoroquinolone |
||
|} |
|} |
||
=== |
===National Hansens's Disease Program (US)=== |
||
{| class="wikitable" |
{| class="wikitable" |
||
! |
!Disease!!Treatment |
||
|- |
|- |
||
| |
|Tuberculoid (TT & BT) (i.e. paucibacillary) |
||
| |
|12 months of [[Is treated by::dapsone]] and [[Is treated by::rifampicin]] |
||
|- |
|- |
||
| |
|Lepromatous (LL, BL, and BB) (i.e. multibacillary) |
||
| |
|24 months of [[Is treated by::dapsone]], [[Is treated by::rifampicin]], and [[Is treated by::clofazimine]] |
||
|} |
|} |
||
=== |
===Second-Line Antibiotics=== |
||
* [[Is treated by::Clarithromycin]] |
|||
* |
*[[Is treated by::Clarithromycin]] |
||
*[[Is treated by::Minocycline]] |
|||
* Fluoroquinolones: [[Is treated by::ofloxacin]], [[Is treated by::levofloxacin]], or [[Is treated by::moxifloxacin]] |
|||
*Fluoroquinolones: [[Is treated by::ofloxacin]], [[Is treated by::levofloxacin]], or [[Is treated by::moxifloxacin]] |
|||
{{DISPLAYTITLE:''Mycobacterium leprae''}} |
{{DISPLAYTITLE:''Mycobacterium leprae''}} |
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Line 105: | Line 142: | ||
[[Category:Mycobacteria]] |
[[Category:Mycobacteria]] |
||
=== |
===Management of Reactions=== |
||
{| class="wikitable" |
{| class="wikitable" |
||
! |
!Reaction!!Management |
||
|- |
|- |
||
| |
|Reversal reaction limited to skin |
||
| |
|monitor clinically |
||
|- |
|- |
||
| |
|Reversal reaction involving nerves |
||
| |
|corticosteroids with slow taper, and [[rifampin]] changed to monthly from daily |
||
|- |
|- |
||
| |
|Other reversal reaction |
||
| |
|corticosteroids based on clinical judgment |
||
|- |
|- |
||
| |
|Erythema nodosum leprosum with neuritis |
||
| |
|[[prednisone]] 1 mg/kg/day (40 to 60 mg/day), tapered over 2 to 4 weeks, possibly with [[thalidomide]] or [[clofazimine]] as a steroid-sparing agent |
||
|- |
|- |
||
| |
|Mild erythema nodosum leprosum |
||
| |
|[[thalidomide]] 50 to 100 mg nightly |
||
|} |
|} |
||
== Prevention == |
|||
* Unclear whether household contacts require prophylaxis[[CiteRef::boodman2021le]] |
|||
** Some experts recommend prophylaxis, particularly for exposure to multibacillary patients |
|||
** Regimen unclear; most Canadian experts use single-dose [[rifampin]], in accordance with WHO recommendations |
|||
** May instead do annual screening by physical examination for between 2 and 10 years |
Latest revision as of 20:01, 5 November 2021
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
Trunk | Palpation | Sensation | Movement | Deformity |
---|---|---|---|---|
Ulnar nerve | Just superior to medial epicondyle | Fifth digit and ulnar aspect of hand | Fifth digit abduction | Claw deformity of little and ring fingers |
Median nerve | Palmar wrist just medial to palmaris longus | Lateral three fingers and palm | Thumb abduction | Claw deformity of first through third digits |
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
Disease | Treatment |
---|---|
Paucibacillary | 6 months of rifampin, dapsone, and clofazimine |
Multibacillary | 12 months of rifampin, dapsone, and clofazimine |
Rifampin resistance | 6 months of at least two second-line drugs (below) with clofazimine, followed by 18 months of one second-line drug with clofazimine |
Quinolone resistance | As for rifampin resistance, but without a fluoroquinolone |
National Hansens's Disease Program (US)
Disease | Treatment |
---|---|
Tuberculoid (TT & BT) (i.e. paucibacillary) | 12 months of dapsone and rifampicin |
Lepromatous (LL, BL, and BB) (i.e. multibacillary) | 24 months of dapsone, rifampicin, and clofazimine |
Second-Line Antibiotics
- Clarithromycin
- Minocycline
- Fluoroquinolones: ofloxacin, levofloxacin, or moxifloxacin
Management of Reactions
Reaction | Management |
---|---|
Reversal reaction limited to skin | monitor clinically |
Reversal reaction involving nerves | corticosteroids with slow taper, and rifampin changed to monthly from daily |
Other reversal reaction | corticosteroids based on clinical judgment |
Erythema nodosum leprosum with neuritis | prednisone 1 mg/kg/day (40 to 60 mg/day), tapered over 2 to 4 weeks, possibly with thalidomide or clofazimine as a steroid-sparing agent |
Mild erythema nodosum leprosum | thalidomide 50 to 100 mg nightly |
Prevention
- Unclear whether household contacts require prophylaxis1
- Some experts recommend prophylaxis, particularly for exposure to multibacillary patients
- Regimen unclear; most Canadian experts use single-dose rifampin, in accordance with WHO recommendations
- May instead do annual screening by physical examination for between 2 and 10 years
References
- ^ boodman2021le