Leptospira: Difference between revisions
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Leptospira
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== |
==Background== |
||
=== |
===Microbiology=== |
||
* Thin, flagellated [[Cellular shape::spirochete]] |
|||
* Best viewed with darkfield microscopy |
|||
* Species and serovars are divided into three broad categories within the genus ''Leptospira'' |
|||
** Pathogens: ''L. interrogans'' (multiple serovars, most common), ''L. noguchii'', ''L. borgpetersenii'', ''L. santarosai'', ''L. kirschneri'', ''L. weilii'', ''L. alexanderi'', ''L. alstonii'', ''L. meyeri'', ''L. wolffi'', and ''L. kmetyi'' |
|||
** Non-pathogenic saprophytes: ''L. biflexa'', ''L. wolbachii'', ''L. vanthielii'', ''L. terpstrae'', ''L. yanagawae'', and ''L. idonii'' |
|||
** Species of indeterminate pathogenicity: ''L. inadai'', ''L. fainei'', ''L. broomii'', and ''L. licerasiae'' |
|||
* Within each species, there may be multiple serovars that are defined based on lipopolysaccharide (LPS) O-antigens |
|||
** A single species may have pathogenic and non-pathogenic serovars |
|||
*Thin, flagellated [[Cellular shape::spirochete]] |
|||
=== Epidemiology === |
|||
*Best viewed with darkfield microscopy |
|||
* Endemic worldwide |
|||
*Species and serovars are divided into three broad categories within the genus ''Leptospira'' |
|||
** More common during rainy seasons in tropical regions and late summer to fall in temperate regions |
|||
**Pathogens: ''L. interrogans'' (multiple serovars, most common), ''L. noguchii'', ''L. borgpetersenii'', ''L. santarosai'', ''L. kirschneri'', ''L. weilii'', ''L. alexanderi'', ''L. alstonii'', ''L. meyeri'', ''L. wolffi'', and ''L. kmetyi'' |
|||
** In US, more common in Hawaii |
|||
**Non-pathogenic saprophytes: ''L. biflexa'', ''L. wolbachii'', ''L. vanthielii'', ''L. terpstrae'', ''L. yanagawae'', and ''L. idonii'' |
|||
* Major reservoir is as a chronic kidney infection in animals, especially rodents |
|||
**Species of indeterminate pathogenicity: ''L. inadai'', ''L. fainei'', ''L. broomii'', and ''L. licerasiae'' |
|||
** Among livestock, may cause spontaneous abortions |
|||
*Within each species, there may be multiple serovars that are defined based on lipopolysaccharide (LPS) O-antigens |
|||
* Most common risk factor is exposure to water or soil contaminated with rodent urine |
|||
**A single species may have pathogenic and non-pathogenic serovars |
|||
** Includes occupational exposures and direct contact |
|||
** High-risk occupations include farmers, slaughterhouse workers, pet traders, veterinarians, rodent catchers and sewer workers |
|||
* Leptospires can survive in water or soil for months, depending on the conditions |
|||
=== |
===Epidemiology=== |
||
* Bacteria enter through cuts and abrasions, mucous membranes, conjunctivae, and inhalation |
|||
* After entering, it disseminates hematogenously |
|||
* Human TLR4 cannot bind leptospiral LPS |
|||
* Virulence factors |
|||
** Sphingomyelinase and hemolysin |
|||
** Also spirochete motility |
|||
** Also hooked ends |
|||
*Endemic worldwide |
|||
== Clinical Manifestations == |
|||
**More common during rainy seasons in tropical regions and late summer to fall in temperate regions |
|||
* Spectrum of severity, from asymptomatic seroconversion (most common) to nonspecific febrile illness to severe, life-threating multiorgan failure |
|||
**In US, more common in Hawaii |
|||
** Asymptomatic disease is likely frequent, given high seroprevalence in some populations |
|||
*Major reservoir is as a chronic kidney infection in animals, especially rodents |
|||
* Incubation period [[Usual incubation period::10 days]] (range [[Incubation period range::5 to 14 days]]) |
|||
**Among livestock, may cause spontaneous abortions |
|||
* '''Acute febrile phase''' |
|||
*Most common risk factor is exposure to water or soil contaminated with rodent urine |
|||
** Acute phase lasts 5 to 7 days |
|||
**Includes occupational exposures and direct contact |
|||
** Starts with high fevers, headaches, chills, rigors, and myalgias |
|||
**High-risk occupations include farmers, slaughterhouse workers, pet traders, veterinarians, rodent catchers and sewer workers |
|||
** Conjunctival injection is an identifying feature |
|||
*Leptospires can survive in water or soil for months, depending on the conditions |
|||
** Muscle tenderness, especially in the calf and lumbar areas, is also characteristic |
|||
** Occasionally have a pretibial papular eruption |
|||
===Pathophysiology=== |
|||
** Can also have lymphadenopathy, splenomegaly, and hepatomegaly |
|||
** Mild leukocytosis and neutrophilia, with thrombocytopenia and occasionally anemia |
|||
*Bacteria enter through cuts and abrasions, mucous membranes, conjunctivae, and inhalation |
|||
** Spirochetes detectable in blood and CSF, possibly urine |
|||
*After entering, it disseminates hematogenously |
|||
* '''Immune phase''' |
|||
*Human TLR4 cannot bind leptospiral LPS |
|||
** Lasts 4 to 30 days |
|||
*Virulence factors |
|||
** Corresponds with the appearance of IgM antibodies |
|||
**Sphingomyelinase and hemolysin |
|||
** Spirochete is cleared from blood and CSF but detectable in other organs, including urine |
|||
**Also spirochete motility |
|||
** May develop jaundice, renal failure, arrhythmias, pulmonary symptoms, [[Causes::aseptic meningitis]], non-purulent conjunctival injection, photophobia, eye pain, muscle tenderness, adenopathy, and [[Causes::hepaosplenomegaly]] |
|||
**Also hooked ends |
|||
* '''Weil disease''' (liver and renal failure) may develop during or directly following the acute phase |
|||
** Liver injury is predominantly jaundice with only mild liver enzyme rise |
|||
==Clinical Manifestations== |
|||
** Renal failure |
|||
*** ''Nonoliguric'' hypokalemia with impaired sodium reabsorption and increased distal sodium delivery |
|||
*Spectrum of severity, from asymptomatic seroconversion (most common) to nonspecific febrile illness to severe, life-threating multiorgan failure |
|||
*** Selective loss of ENaC channels in proximal ubule |
|||
**Asymptomatic disease is likely frequent, given high seroprevalence in some populations |
|||
*** Biopsy shows AIN |
|||
*Incubation period [[Usual incubation period::10 days]] (range [[Incubation period range::5 to 14 days]]) |
|||
* '''Severe pulmonary hemorrhage syndrome''' (SPHS) |
|||
*'''Acute febrile phase''' |
|||
** May have frank hemoptysis, but not always |
|||
**Acute phase lasts 5 to 7 days |
|||
** Can show up as CXR lower lobe "snowflake-like" densities |
|||
**Starts with high [[fever]], [[headache]], chills, rigors, and [[myalgias]] |
|||
* Arrhythmias, including atrial fibrillation and ventricular tachycardia |
|||
**Conjunctival injection is an identifying feature |
|||
* Circulatory shock |
|||
**Muscle tenderness, especially in the calf and lumbar areas, is also characteristic |
|||
** Rarely, congestive heart failure from myocarditis |
|||
**Occasionally have a pretibial papular eruption |
|||
* Severe disease has high mortality from 5 to 40% |
|||
**Can also have [[lymphadenopathy]], [[splenomegaly]], and [[hepatomegaly]] |
|||
**Mild leukocytosis and neutrophilia, with thrombocytopenia and occasionally anemia |
|||
**Spirochetes detectable in blood and CSF, possibly urine |
|||
*'''Immune phase''' |
|||
**Lasts 4 to 30 days |
|||
**Corresponds with the appearance of IgM antibodies |
|||
**Spirochete is cleared from blood and CSF but detectable in other organs, including urine |
|||
**May develop [[Causes::jaundice]], [[Causes::acute renal failure]], [[Causes::arrhythmias]], pulmonary symptoms, [[Causes::aseptic meningitis]], [[Causes::non-purulent conjunctival injection]], [[Causes::photophobia]], eye pain, muscle tenderness, [[Causes::adenopathy]], and [[Causes::hepaosplenomegaly|Causes::hepatosplenomegaly]] |
|||
*'''Weil disease''' (liver and renal failure) may develop during or directly following the acute phase |
|||
**Liver injury is predominantly [[jaundice]] with only mild liver enzyme rise |
|||
**Renal failure |
|||
***''Nonoliguric'' hypokalemia with impaired sodium reabsorption and increased distal sodium delivery |
|||
***Selective loss of ENaC channels in proximal ubule |
|||
***Biopsy shows AIN |
|||
*'''Severe pulmonary hemorrhage syndrome''' (SPHS) |
|||
**May have frank [[hemoptysis]], but not always |
|||
**Can show up as CXR lower lobe "snowflake-like" densities |
|||
*Arrhythmias, including atrial fibrillation and ventricular tachycardia |
|||
*Circulatory shock |
|||
**Rarely, congestive heart failure from myocarditis |
|||
*Severe disease has high mortality from 5 to 40% |
|||
==Diagnosis== |
|||
*In general, use PCR if early in disease (<7 days) and ELISA IgM followed by confirmatory MAT if further in disease (≥7 days) |
|||
== Diagnosis == |
|||
* In general, use PCR if early in disease (<7 days) and ELISA IgM followed by confirmatory MAT if further in disease (≥7 days) |
|||
{| class="wikitable" |
{| class="wikitable" |
||
! |
!Method!!Sens!!Spec |
||
|- |
|- |
||
| |
|Culture||5-50%||100% |
||
|- |
|- |
||
| |
|Darkfield microscopy||40%||60% |
||
|- |
|- |
||
| |
|Microscopic agglutination test (MAT)||90%||>90% |
||
|- |
|- |
||
| |
|ELISA IgM||>90%||88-95% |
||
|- |
|- |
||
| |
|Latex agglutination||92%||95% |
||
|- |
|- |
||
| |
|Lateral flow assay||81%||96% |
||
|- |
|- |
||
| |
|PCR||100%||93% |
||
|} |
|} |
||
=== |
===Microscopy=== |
||
* Leptospires can be seen directly under darkfield microscopy |
|||
*Leptospires can be seen directly under darkfield microscopy |
|||
* Low sensitivity and specificity of blood and urine samples, even if spirochetes are seen (as spirochetes can also be normal flora) |
|||
*Low sensitivity and specificity of blood and urine samples, even if spirochetes are seen (as spirochetes can also be normal flora) |
|||
===Culture=== |
|||
*Can get positive cultures from blood and CSF, ideally when collected while febrile and before antibiotics |
|||
*Can inoculate one to blood drops directly into culture at bedside |
|||
*Urine can be cultured after the first week of illness, but need to be processed quickly |
|||
*Use Fletcher's medium (commercial version) |
|||
*Not very sensitive, and cultures can take weeks |
|||
===Serology=== |
|||
*Detects IgM antibodies, which appear around day 5 to 7 |
|||
*Microscopic agglutination test (MAT) for antigen detection (Sn 90%, Sp 90%) |
|||
**''Leptospira'' antigens are mixed with serum and monitored for agglutination |
|||
**Monitor for a four-fold rise in titres from acute-phase to convalescent phase (repeat 4 to 6 weeks), or a single titre of at least 1:800 |
|||
**May cross-react with [[syphilis]], [[relapsing fever]], [[Lyme disease]], [[viral hepatitis]], HIV, [[Legionella]], and autoimmune diseases |
|||
**Cross-reacts between different serogroups |
|||
*IgM ELISA, needs confirmation by MAT (Sn 90%, Sp 90%) (this is the test in Canada) |
|||
*Latex agglutination test, needs confirmation by MAT (Sn 80%, Sp 95%) |
|||
*Lateral flow test, needs confirmation by MAT (Sn 80%, Sp 95%) |
|||
===PCR=== |
|||
*Loop-mediated isothermal amplification (LAMP) assays and other PCR assays exist |
|||
*Unclear sensitivity and specificity, but has the potential to diagnose disease before antibodies develop |
|||
*Usually done from blood, but can try in urine as well |
|||
==Differential Diagnosis== |
|||
=== Culture === |
|||
* Can get positive cultures from blood and CSF, ideally when collected while febrile and before antibiotics |
|||
* Can inoculate one to blood drops directly into culture at bedside |
|||
* Urine can be cultured after the first week of illness, but need to be processed quickly |
|||
* Use Fletcher's medium (commercial version) |
|||
* Not very sensitive, and cultures can take weeks |
|||
*Early in disease, it is essentially a non-specific febrile syndrome |
|||
=== Serology === |
|||
*'''Viral''' |
|||
* Detects IgM antibodies, which appear around day 5 to 7 |
|||
**[[Influenza]] |
|||
* Microscopic agglutination test (MAT) for antigen detection (Sn 90%, Sp 90%) |
|||
**Acute [[HIV]] |
|||
** ''Leptospira'' antigens are mixed with serum and monitored for agglutination |
|||
**[[Infectious mononucleosis]] ([[EBV]]/[[CMV]]) |
|||
** Monitor for a four-fold rise in titres from acute-phase to convalescent phase (repeat 4 to 6 weeks), or a single titre of at least 1:800 |
|||
**Flaviviruses: [[dengue virus]], [[yellow fever virus]], [[West Nile virus]] |
|||
** May cross-react with [[syphilis]], [[relapsing fever]], [[Lyme disease]], [[viral hepatitis]], HIV, [[Legionella]], and autoimmune diseases |
|||
**Alphaviruses: [[Chikungunya virus]] |
|||
** Cross-reacts between different serogroups |
|||
**Bunyaviruses: [[Hantavirus]], [[Lassa fever virus]] |
|||
* IgM ELISA, needs confirmation by MAT (Sn 90%, Sp 90%) (this is the test in Canada) |
|||
**Other [[viral hemorrhagic fever virus]] |
|||
* Latex agglutination test, needs confirmation by MAT (Sn 80%, Sp 95%) |
|||
**[[Viral hepatitis]] |
|||
* Lateral flow test, needs confirmation by MAT (Sn 80%, Sp 95%) |
|||
**[[Measles virus]], with cough and conjunctivitis |
|||
*'''Bacterial''' |
|||
**[[Rickettsioses]], including [[Rocky Mountain spotted fever]] |
|||
**[[Borreliosis]] |
|||
**[[Brucella]] |
|||
**[[Enteric fever]] |
|||
*'''Parasitic''' |
|||
**[[Malaria]] |
|||
== |
==Management== |
||
* Loop-mediated isothermal amplification (LAMP) assays and other PCR assays exist |
|||
* Unclear sensitivity and specificity, but has the potential to diagnose disease before antibodies develop |
|||
* Usually done from blood, but can try in urine as well |
|||
*Treat early in disease course, usually before diagnosis |
|||
== Differential Diagnosis == |
|||
*Usual treatment is [[Is treated by::penicillin]] G 1.5 MU IV q6h, if severe, or [[Is treated by::doxycycline]] 100 mg po bid, if mild |
|||
* Early in disease, it is essentially a non-specific febrile syndrome |
|||
**May be able to use [[Is treated by::amoxicillin]], [[Is treated by::ampicillin]], [[Is treated by::ceftriaxone]], or [[Is treated by::azithromycin]] as alternatives |
|||
* '''Viral''' |
|||
**May develop a Jarisch-Herxheimer reaction during treatment (only with beta-lactams) |
|||
** [[Influenza]] |
|||
**Duration is 5 to 7 days (except 3 days for [[azithromycin]] |
|||
** Acute [[HIV]] |
|||
*Close monitor and intensive supportive therapy required for severe patient |
|||
** [[Infectious mononucleosis]] ([[EBV]]/[[CMV]]) |
|||
*May need hemodialysis, but usually recovers renal function |
|||
** Flaviviruses: [[dengue virus]], [[yellow fever virus]], [[West Nile virus]] |
|||
*SPHS is managed as ARDS with lung-protective ventilation |
|||
** Alphaviruses: [[Chikungunya virus]] |
|||
** Bunyaviruses: [[Hantavirus]], [[Lassa fever virus]] |
|||
** Other [[viral hemorrhagic fever virus]] |
|||
** [[Viral hepatitis]] |
|||
** [[Measles virus]], with cough and conjunctivitis |
|||
* '''Bacterial''' |
|||
** [[Rickettsioses]], including [[Rocky Mountain spotted fever]] |
|||
** [[Borreliosis]] |
|||
** [[Brucella]] |
|||
** [[Enteric fever]] |
|||
* '''Parasitic''' |
|||
** [[Malaria]] |
|||
== |
==Prevention== |
||
* Treat early in disease course, usually before diagnosis |
|||
* Usual treatment is [[Is treated by::penicillin]] G 1.5 MU IV q6h, if severe, or [[Is treated by::doxycycline]] 100 mg po bid, if mild |
|||
** May be able to use [[Is treated by::amoxicillin]], [[Is treated by::ampicillin]], [[Is treated by::ceftriaxone]], or [[Is treated by::azithromycin]] as alternatives |
|||
** May develop a Jarisch-Herxheimer reaction during treatment (only with beta-lactams) |
|||
** Duration is 5 to 7 days (except 3 days for [[azithromycin]] |
|||
* Close monitor and intensive supportive therapy required for severe patient |
|||
* May need hemodialysis, but usually recovers renal function |
|||
* SPHS is managed as ARDS with lung-protective ventilation |
|||
*Mostly avoidance of high-risk exposures |
|||
== Prevention == |
|||
*Immunization is possible but rarely done, and covers only specific serovars |
|||
* Mostly avoidance of high-risk exposures |
|||
**Even if immunizing animals, it prevents disease but not asymptomatic carriage |
|||
* Immunization is possible but rarely done, and covers only specific serovars |
|||
*Can do chemoprophylaxis of high risk occupations with [[doxycycline]] 200 mg PO once weekly |
|||
** Even if immunizing animals, it prevents disease but not asymptomatic carriage |
|||
* Can do chemoprophylaxis of high risk occupations with [[doxycycline]] 200 mg PO once weekly |
|||
{{DISPLAYTITLE:''Leptospira'' species}} |
{{DISPLAYTITLE:''Leptospira'' species}} |
||
Revision as of 21:19, 10 August 2020
Background
Microbiology
- Thin, flagellated spirochete
- Best viewed with darkfield microscopy
- Species and serovars are divided into three broad categories within the genus Leptospira
- Pathogens: L. interrogans (multiple serovars, most common), L. noguchii, L. borgpetersenii, L. santarosai, L. kirschneri, L. weilii, L. alexanderi, L. alstonii, L. meyeri, L. wolffi, and L. kmetyi
- Non-pathogenic saprophytes: L. biflexa, L. wolbachii, L. vanthielii, L. terpstrae, L. yanagawae, and L. idonii
- Species of indeterminate pathogenicity: L. inadai, L. fainei, L. broomii, and L. licerasiae
- Within each species, there may be multiple serovars that are defined based on lipopolysaccharide (LPS) O-antigens
- A single species may have pathogenic and non-pathogenic serovars
Epidemiology
- Endemic worldwide
- More common during rainy seasons in tropical regions and late summer to fall in temperate regions
- In US, more common in Hawaii
- Major reservoir is as a chronic kidney infection in animals, especially rodents
- Among livestock, may cause spontaneous abortions
- Most common risk factor is exposure to water or soil contaminated with rodent urine
- Includes occupational exposures and direct contact
- High-risk occupations include farmers, slaughterhouse workers, pet traders, veterinarians, rodent catchers and sewer workers
- Leptospires can survive in water or soil for months, depending on the conditions
Pathophysiology
- Bacteria enter through cuts and abrasions, mucous membranes, conjunctivae, and inhalation
- After entering, it disseminates hematogenously
- Human TLR4 cannot bind leptospiral LPS
- Virulence factors
- Sphingomyelinase and hemolysin
- Also spirochete motility
- Also hooked ends
Clinical Manifestations
- Spectrum of severity, from asymptomatic seroconversion (most common) to nonspecific febrile illness to severe, life-threating multiorgan failure
- Asymptomatic disease is likely frequent, given high seroprevalence in some populations
- Incubation period 10 days (range 5 to 14 days)
- Acute febrile phase
- Acute phase lasts 5 to 7 days
- Starts with high fever, headache, chills, rigors, and myalgias
- Conjunctival injection is an identifying feature
- Muscle tenderness, especially in the calf and lumbar areas, is also characteristic
- Occasionally have a pretibial papular eruption
- Can also have lymphadenopathy, splenomegaly, and hepatomegaly
- Mild leukocytosis and neutrophilia, with thrombocytopenia and occasionally anemia
- Spirochetes detectable in blood and CSF, possibly urine
- Immune phase
- Lasts 4 to 30 days
- Corresponds with the appearance of IgM antibodies
- Spirochete is cleared from blood and CSF but detectable in other organs, including urine
- May develop jaundice, acute renal failure, arrhythmias, pulmonary symptoms, aseptic meningitis, non-purulent conjunctival injection, photophobia, eye pain, muscle tenderness, adenopathy, and Causes::hepatosplenomegaly
- Weil disease (liver and renal failure) may develop during or directly following the acute phase
- Liver injury is predominantly jaundice with only mild liver enzyme rise
- Renal failure
- Nonoliguric hypokalemia with impaired sodium reabsorption and increased distal sodium delivery
- Selective loss of ENaC channels in proximal ubule
- Biopsy shows AIN
- Severe pulmonary hemorrhage syndrome (SPHS)
- May have frank hemoptysis, but not always
- Can show up as CXR lower lobe "snowflake-like" densities
- Arrhythmias, including atrial fibrillation and ventricular tachycardia
- Circulatory shock
- Rarely, congestive heart failure from myocarditis
- Severe disease has high mortality from 5 to 40%
Diagnosis
- In general, use PCR if early in disease (<7 days) and ELISA IgM followed by confirmatory MAT if further in disease (≥7 days)
| Method | Sens | Spec |
|---|---|---|
| Culture | 5-50% | 100% |
| Darkfield microscopy | 40% | 60% |
| Microscopic agglutination test (MAT) | 90% | >90% |
| ELISA IgM | >90% | 88-95% |
| Latex agglutination | 92% | 95% |
| Lateral flow assay | 81% | 96% |
| PCR | 100% | 93% |
Microscopy
- Leptospires can be seen directly under darkfield microscopy
- Low sensitivity and specificity of blood and urine samples, even if spirochetes are seen (as spirochetes can also be normal flora)
Culture
- Can get positive cultures from blood and CSF, ideally when collected while febrile and before antibiotics
- Can inoculate one to blood drops directly into culture at bedside
- Urine can be cultured after the first week of illness, but need to be processed quickly
- Use Fletcher's medium (commercial version)
- Not very sensitive, and cultures can take weeks
Serology
- Detects IgM antibodies, which appear around day 5 to 7
- Microscopic agglutination test (MAT) for antigen detection (Sn 90%, Sp 90%)
- Leptospira antigens are mixed with serum and monitored for agglutination
- Monitor for a four-fold rise in titres from acute-phase to convalescent phase (repeat 4 to 6 weeks), or a single titre of at least 1:800
- May cross-react with syphilis, relapsing fever, Lyme disease, viral hepatitis, HIV, Legionella, and autoimmune diseases
- Cross-reacts between different serogroups
- IgM ELISA, needs confirmation by MAT (Sn 90%, Sp 90%) (this is the test in Canada)
- Latex agglutination test, needs confirmation by MAT (Sn 80%, Sp 95%)
- Lateral flow test, needs confirmation by MAT (Sn 80%, Sp 95%)
PCR
- Loop-mediated isothermal amplification (LAMP) assays and other PCR assays exist
- Unclear sensitivity and specificity, but has the potential to diagnose disease before antibodies develop
- Usually done from blood, but can try in urine as well
Differential Diagnosis
- Early in disease, it is essentially a non-specific febrile syndrome
- Viral
- Influenza
- Acute HIV
- Infectious mononucleosis (EBV/CMV)
- Flaviviruses: dengue virus, yellow fever virus, West Nile virus
- Alphaviruses: Chikungunya virus
- Bunyaviruses: Hantavirus, Lassa fever virus
- Other viral hemorrhagic fever virus
- Viral hepatitis
- Measles virus, with cough and conjunctivitis
- Bacterial
- Parasitic
Management
- Treat early in disease course, usually before diagnosis
- Usual treatment is penicillin G 1.5 MU IV q6h, if severe, or doxycycline 100 mg po bid, if mild
- May be able to use amoxicillin, ampicillin, ceftriaxone, or azithromycin as alternatives
- May develop a Jarisch-Herxheimer reaction during treatment (only with beta-lactams)
- Duration is 5 to 7 days (except 3 days for azithromycin
- Close monitor and intensive supportive therapy required for severe patient
- May need hemodialysis, but usually recovers renal function
- SPHS is managed as ARDS with lung-protective ventilation
Prevention
- Mostly avoidance of high-risk exposures
- Immunization is possible but rarely done, and covers only specific serovars
- Even if immunizing animals, it prevents disease but not asymptomatic carriage
- Can do chemoprophylaxis of high risk occupations with doxycycline 200 mg PO once weekly
