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MENINGITIS
Introduction
Bacterial meningitis is an acute purulent infection within the sub-arachnoid space , associated with a CNS inflammatory reaction.
• The organisms most often responsible for community- acquired bacterial meningitis are : Streptococcus pneumoniae (50%) Neisseria meningitidis (25%) Group B streptococci (15%) Listeria monocytogenes (10%) Haemophilus influenzae type b (<10%) N. meningitidis is the causative organism of recurring epidemics of meningitis every 8 to 12 years.
• S. pneumoniae is the most common cause of meningitis in adults >20 years of age Predisposing conditions: - Pneumococcal pneumonia - coexisting acute or chronic pneumococcal sinusitis or otitis media - Alcoholism - Diabetes -Splenectomy,hypogammaglobulinemia, complement deficiency -Head trauma with basilar skull fracture and CSF rhinorrhea
• The incidence of meningitis due to N. meningitidis has decreased with the routine immunization of 11- to 18-year-olds with the tetravalent (serogroups A, C, W-135, and Y) meningococcal glycoconjugate vaccine. • The vaccine does not contain serogroup B, which is responsible for one-third of cases of meningococcal disease. • The presence of petechial or purpuric skin lesions can provide an important clue to the diagnosis of meningococcal infection.
• Enteric gram-negative bacilli cause meningitis in individuals with chronic and debilitating diseases such as diabetes, cirrhosis, or alcoholism and in those with chronic urinary tract infections and can also complicate neurosurgical procedures, particularly craniotomy.
• Group B streptococcus, or S. agalactiae, was previously responsible for meningitis predominantly in neonates, but it has been reported with increasing frequency in individuals >50 years of age. • The frequency of H. influenzae type b meningitis in children has declined dramatically since the introduction of the Hib conjugate vaccine. Non-b H. influenzae is an emerging pathogen.
• L. monocytogenes in - neonates (<1 month of age) - pregnant women - individuals >60 years - immunocompromised individuals of all ages. Infection is acquired by ingesting contaminated coleslaw, milk, soft cheeses, and several types of "ready-to-eat" foods.
• Staphylococcus aureus and coagulase- negative staphylococci following invasive neurosurgical procedures, particularly shunting procedures.
PATHOPHYSIOLOGY • Bacteria are able to avoid phagocytosis by neutrophils and classic complement-mediated bactericidal activity because of the presence of a polysaccharide capsule multiply rapidly within CSF because of the absence of effective host immune defenses. • Normal CSF contains few white blood cells (WBCs) and relatively small amounts of complement proteins and immunoglobulins - prevents effective opsonization of bacteria, an essential prerequisite for bacterial phagocytosis by neutrophils. • Phagocytosis of bacteria is further impaired by the fluid nature of CSF, which is less conducive to phagocytosis than a solid tissue substrate.
CLINICAL PRESENTATION • Classic clinical triad of meningitis is fever, headache, and nuchal rigidity, but the classic triad may not be present. • A decreased level of consciousness (>75%) • Nausea, vomitting, photophobia • Seizures (20–40%) • Focal seizures are usually due to focal arterial ischemia or infarction, cortical venous thrombosis with hemorrhage, or focal edema. • Generalized seizure activity and status epilepticus may be due to hyponatremia, cerebral anoxia, or, less commonly, the toxic effects of antimicrobial agents such as high-dose penicillin.
• The CSF LA test has a specificity of 95–100% for S. pneumoniae and N. meningitidis. • Sensitivity of the CSF LA test is only 70–100% for detection of S. pneumoniae and 33–70% for detection of N. meningitidis antigens, so a negative test does not exclude infection by these organisms. • Limulus amebocyte lysate assay has a specificity of 85–100% and a sensitivity approaching 100%.
Relationship between Cerebrospinal Fluid Glucose and Serum Glucose N Engl J Med 2012; 366:576-578February 9, 2012DOI: 10.1056/NEJMc1111080 • Bacterial meningitis typically have low levels of CSF glucose because of glycolysis by both white cells and the pathogen and impaired CSF glucose transport. • Level of CSF glucose is typically interpreted in relation to that of serum glucose, since glucose passes across the blood–brain barrier. Standard reference texts cite the normal ratio of CSF to serum glucose as 0.6,4 although this ratio has not been rigorously investigated. • Specifically, the normal level of CSF glucose should be approximately 60% of the level of serum glucose.
EMPIRICAL ANTIMICROBIAL TREATMENT • Goal is to begin antimicrobial therapy within 60 minutes of patient’s arrival in the emergency room. • S. pneumoniae and N. meningitidis are the most common etiologic organisms of community-acquired bacterial meningitis.
• Due to the emergence of penicillin- and cephalosporin-resistant S. pneumoniae, empirical therapy of community-acquired suspected bacterial meningitis in children and adults should include a combination of 1. Dexamethasone 2. Third- or fourth-generation cephalosporin (e.g., ceftriaxone, cefotaxime, or cefepime) 3. Vancomycin 4. Acyclovir, as HSV encephalitis is the leading disease in the differential diagnosis 5. Doxycycline during tick season in endemic area
• Ceftriaxone or cefotaxime provide good coverage for - susceptible S. pneumoniae - group B streptococci - H. influenzae Adequate coverage for N. meningitidis • Cefepime is a broad-spectrum fourth-generation cephalosporin - in vitro activity similar to that of cefotaxime or ceftriaxone against S. pneumoniae and N. meningitidis -greater activity against Enterobacter species and Pseudomonas aeruginosa
• Ampicillin should be added to the empirical regimen for coverage of L. monocytogenes in - individuals <3 months of age - adults >55 - with suspected impaired cell-mediated immunity because of chronic illness, organ transplantation, pregnancy, malignancy, or immunosuppressive therapy • Metronidazole is added to the empirical regimen to cover gram-negative anaerobes in patients with otitis, sinusitis, or mastoiditis.
• In hospital-acquired meningitis, and particularly meningitis following neurosurgical procedures, staphylococci and gram- negative organisms including P. aeruginosa are the most common etiologic organisms. • Empirical therapy – - combination of vancomycin and ceftazidime, cefepime, or meropenem. - Ceftazidime, cefepime, or meropenem should be substituted for ceftriaxone or cefotaxime in neurosurgical patients and in neutropenic patients, as ceftriaxone and cefotaxime do not provide adequate activity against CNS infection with P. aeruginosa. - Meropenem is a carbapenem antibiotic that is highly active in vitro against L. monocytogenes, has been demonstrated to be effective in cases of meningitis caused by P. aeruginosa, and shows good activity against penicillin-resistant pneumococci.
Specific Antimicrobial Therapy • Pneumococcal Meningitis - cephalosporin (ceftriaxone, cefotaxime, or cefepime) and vancomycin - Rifampin can be added to vancomycin for its synergistic effect but is inadequate as monotherapy because resistance develops rapidly when it is used alone. -2-week course of intravenous antimicrobial therapy is recommended. - Repeat LP performed 24–36 h after the initiation of antimicrobial therapy to document sterilization of the CSF. - Failure to sterilize the CSF after 24–36 h of antibiotic therapy should be considered presumptive evidence of antibiotic resistance. Patients may benefit from the addition of intraventricular vancomycin.
• Meningococcal Meningitis - Penicillin G remains the antibiotic of choice for susceptible strains. - Ceftriaxone and cefotaxime provide adequate empirical coverage. - Isolates of N. meningitidis with moderate resistance to penicillin have still been successfully treated with penicillin. - A 7-day course of intravenous antibiotic therapy is adequate for uncomplicated meningococcal meningitis.
Chemoprophylaxis for the close contacts • Close contacts are defined as those individuals who have had contact with oropharyngeal secretions, either through kissing or by sharing toys, beverages, or cigarettes. • 2-day regimen of rifampin (600 mg every 12 h for 2 days in adults and 10 mg/kg every 12 h for 2 days in children >1 year). Rifampin is not recommended in pregnant women. • Alternatively, adults can be treated with one dose of azithromycin (500 mg), or one intramuscular dose of ceftriaxone (250 mg).
• Listeria Meningitis - Ampicillin for at least 3 weeks. - Gentamicin is added in critically ill patients (2 mg/kg loading dose, then 7.5 mg/kg per day given every 8 h). - Trimethoprim (10–20 mg/kg per day) and sulfamethoxazole (50–100 mg/kg per day) given every 6 h may provide an alternative in penicillin- allergic patients.
• Staphylococcal Meningitis -Susceptible strains of S. aureus or coagulase- negative staphylococci is treated with nafcillin. -Vancomycin is the drug of choice for methicillin- resistant staphylococci and for patients allergic to penicillin. -If the CSF is not sterilized after 48 h of intravenous vancomycin therapy, then either intraventricular or intrathecal vancomycin, 20 mg once daily, can be added.
• Gram-Negative Bacillary Meningitis - The third-generation cephalosporins— cefotaxime, ceftriaxone, and ceftazidime, with the exception of meningitis due to P. aeruginosa, which should be treated with ceftazidime, cefepime, or meropenem - 3-week course of intravenous antibiotic therapy is recommended
Adjunctive Therapy • The release of bacterial cell-wall components by bactericidal antibiotics inflammatory cytokines IL-1 and TNF- in the subarachnoid space. • Dexamethasone - inhibits the synthesis of IL-1 and TNF - decreases CSF outflow resistance - stabilizes the blood-brain barrier
• The results of clinical trials of dexamethasone therapy in children, predominantly with meningitis due to H. influenzae and S. pneumoniae, have demonstrated its efficacy in decreasing meningeal inflammation and incidence of sensorineural hearing loss. • A prospective European trial of adjunctive therapy for acute bacterial meningitis in 301 adults found that dexamethasone reduced the number of unfavorable outcomes (15 vs. 25%, p = .03) including death (7 vs. 15%, p = .04) • Dexamethasone (10 mg intravenously) was administered 15–20 min before the first dose of an antimicrobial agent, and the same dose was repeated every 6 h for 4 days.
• Therapy with dexamethasone should ideally be started 20 min before, or not later than concurrent with, the first dose of antibiotics. • It is unlikely to be of significant benefit if started >6 h after antimicrobial therapy has been initiated. • Dexamethasone may decrease the penetration of vancomycin into CSF. • The rationale for giving dexamethasone 20 min before antibiotic therapy is that dexamethasone inhibits the production of TNF- by macrophages and microglia only if it is administered before these cells are activated by endotoxin. Dexamethasone does not alter TNF- production once it has been induced.
• In experimental models of meningitis, dexamethasone therapy increased hippocampal cell injury and reduced learning capacity. This has not been the case in clinical series. • . Three large randomized trials in low-income countries (sub-Saharan Africa, Southeast Asia) failed to show benefit in subgroups of patients. - Attributed to late presentation to the hospital with more advanced disease, antibiotic pretreatment, malnutrition, infection with HIV. - The results of these clinical trials suggest that patients in sub-Saharan Africa and those in low-income countries with negative CSF Gram's stain and culture should not be treated with dexamethasone.
VIRAL MENINGITIS • Headache, fever, and signs of meningeal irritation. • Frontal or retroorbital pain, photophobia and pain on moving the eyes. • Constitutional signs can include malaise, myalgia, anorexia, nausea and vomiting, abdominal pain, and/or diarrhea.
Etiology • Enteroviruses (including echoviruses and coxsackieviruses) • HSV type 2 (HSV-2) • HIV • arboviruses Approximately two-thirds of culture- negative cases of "aseptic" meningitis have a specific viral etiology identified by CSF PCR testing.
Laboratory Diagnosis CSF Examination - lymphocytic pleocytosis (25–500 cells/L) - normal or slightly elevated protein concentration] - normal glucose concentration - Organisms are not seen on Gram's stain of CSF. - Rarely, PMNs may predominate in the first 48 h of illness, especially with infections due to echovirus 9, West Nile virus, eastern equine encephalitis (EEE) virus, or mumps. - The CSF glucose concentration may be decreased in 10–30% of cases due to mumps or LCMV. As a rule, a lymphocytic pleocytosis with a low glucose concentration should suggest fungal or tuberculous meningitis, Listeria meningoencephalitis, or noninfectious disorders (e.g., sarcoid, neoplastic meningitis).
Polymerase Chain Reaction Amplification of Viral Nucleic Acid - In both enteroviral and HSV infections of the CNS, PCR has become the diagnostic procedure of choice. - HSV PCR is also an important diagnostic test in patients with recurrent episodes of "aseptic" meningitis, many of whom have amplifiable HSV DNA in CSF despite negative viral cultures. - CSF PCR tests are available for WNV but are not as sensitive as detection of WNV-specific CSF IgM. - PCR is also useful in the diagnosis of CNS infection caused by Mycoplasma pneumoniae, which can mimic viral meningitis and encephalitis.
Viral Culture • The sensitivity of CSF cultures, in contrast to its utility in bacterial infections, is generally poor. Serologic Studies • For some viruses, including many arboviruses such as WNV, serologic studies remain a crucial diagnostic tool. • Less useful for viruses with high seroprevalence rates in the general population such as HSV, VZV, CMV, and EBV. • CSF oligoclonal gamma globulin bands occur in association with a number of viral infections,also occur commonly in certain noninfectious neurologic diseases (e.g., multiple sclerosis) and nonviral infections (e.g., neurosyphilis, Lyme neuroborreliosis).
TREATMENT • Symptomatic Rx - analgesics, antipyretics, and antiemetics. Fluid and electrolyte status should be monitored. • Oral or intravenous acyclovir – HSV-1 or -2 severe EBV or VZV infection • Seriously ill patients – intravenous acyclovir (15–30 mg/kg per day in three divided doses), which can be followed by an oral drug such as acyclovir (800 mg, five times daily), famciclovir (500 mg tid), or valacyclovir (1000 mg tid) for a total course of 7–14 days. • Patients who are less ill can be treated with oral drugs alone.
SUBACUTE MENINGITIS • Unrelenting headache, stiff neck, low-grade fever, and lethargy for days to several weeks before they present for evaluation. • Cranial nerve abnormalities and night sweats may be present. ETIOLOGY • M. Tuberculosis • C. neoformans • C. Immitis • T. Pallidum
Laboratory Diagnosis CSF : (1) elevated opening pressure (2) lymphocytic pleocytosis (10–500 cells/L) (3) elevated protein concentration 4) decreased glucose • Positive AFB smears - 10–40% of cases of tuberculous meningitis in adults. • Cultures of CSF for TB are positive in 50% of adults. Culture remains the gold standard to make the diagnosis of tuberculous meningitis. • PCR for the detection of M. tuberculosis DNA - sensitivity and specificity on CSF have not been defined. • The Centers for Disease Control and Prevention recommend the use of nucleic acid amplification tests for the diagnosis of pulmonary tuberculosis.
• CSF abnormalities in fungal meningitis are a mononuclear or lymphocytic pleocytosis, an increased protein concentration, and a decreased glucose concentration. • There may be eosinophils in the CSF in C. immitis meningitis. • The cryptococcal polysaccharide antigen test is a highly sensitive and specific test for cryptococcal meningitis. • The detection of the histoplasma polysaccharide antigen in CSF establishes the diagnosis of a fungal meningitis but is not specific for meningitis due to H. capsulatum. It may be falsely positive in coccidioidal meningitis.
Empirical therapy of tuberculous meningitis • Isoniazid (300 mg/d), Rifampin (10 mg/kg per day), Pyrazinamide (30 mg/kg per day in divided doses), Ethambutol (15–25 mg/kg per day in divided doses), and pyridoxine (50 mg/d). • If the clinical response is good, pyrazinamide can be discontinued after 8 weeks and isoniazid and rifampin continued alone for the next 6–12 months. • A 6-month course of therapy is acceptable, but therapy should be prolonged for 9–12 months in patients who have an inadequate resolution of symptoms of meningitis or who have positive mycobacterial cultures of CSF during the course of therapy. • Dexamethasone therapy is recommended for HIV-negative patients with tuberculous meningitis. • The dose is 12–16 mg per day for 3 weeks, then tapered over 3 weeks.
Meningitis due to C. neoformans in non-HIV, nontransplant patients • Induction therapy - amphotericin B (AmB) (0.7 mg/kg IV per day) plus flucytosine (100 mg/kg per day in four divided doses) for at least 4 weeks if CSF culture results are negative after 2 weeks of treatment. • Therapy should be extended for a total of 6 weeks in the patient with neurologic complications. • Consolidation therapy - fluconazole 400 mg per day for 8 weeks.
Organ transplant recipients/ HIV infected : • liposomal AmB (3–4 mg/kg per day) or AmB lipid complex (ABLC) 5 mg/kg per day plus flucytosine (100 mg/kg per day in four divided doses) for at least 2 weeks or until CSF culture is sterile. • Followed by an 8- to 10-week course of fluconazole [400–800 mg/d (6–12 mg/kg) PO]. • If the CSF culture is sterile after 10 weeks of acute therapy, the dose of fluconazole is decreased to 200 mg/d for 6 months to a year. • HIV-infected patients may require indefinite maintenance therapy with fluconazole 200 mg/day.
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  • 3. Bacterial meningitis is an acute purulent infection within the sub-arachnoid space , associated with a CNS inflammatory reaction.
  • 4. • The organisms most often responsible for community- acquired bacterial meningitis are : Streptococcus pneumoniae (50%) Neisseria meningitidis (25%) Group B streptococci (15%) Listeria monocytogenes (10%) Haemophilus influenzae type b (<10%) N. meningitidis is the causative organism of recurring epidemics of meningitis every 8 to 12 years.
  • 5. • S. pneumoniae is the most common cause of meningitis in adults >20 years of age Predisposing conditions: - Pneumococcal pneumonia - coexisting acute or chronic pneumococcal sinusitis or otitis media - Alcoholism - Diabetes -Splenectomy,hypogammaglobulinemia, complement deficiency -Head trauma with basilar skull fracture and CSF rhinorrhea
  • 6. • The incidence of meningitis due to N. meningitidis has decreased with the routine immunization of 11- to 18-year-olds with the tetravalent (serogroups A, C, W-135, and Y) meningococcal glycoconjugate vaccine. • The vaccine does not contain serogroup B, which is responsible for one-third of cases of meningococcal disease. • The presence of petechial or purpuric skin lesions can provide an important clue to the diagnosis of meningococcal infection.
  • 7. • Enteric gram-negative bacilli cause meningitis in individuals with chronic and debilitating diseases such as diabetes, cirrhosis, or alcoholism and in those with chronic urinary tract infections and can also complicate neurosurgical procedures, particularly craniotomy.
  • 8. • Group B streptococcus, or S. agalactiae, was previously responsible for meningitis predominantly in neonates, but it has been reported with increasing frequency in individuals >50 years of age. • The frequency of H. influenzae type b meningitis in children has declined dramatically since the introduction of the Hib conjugate vaccine. Non-b H. influenzae is an emerging pathogen.
  • 9. • L. monocytogenes in - neonates (<1 month of age) - pregnant women - individuals >60 years - immunocompromised individuals of all ages. Infection is acquired by ingesting contaminated coleslaw, milk, soft cheeses, and several types of "ready-to-eat" foods.
  • 10. • Staphylococcus aureus and coagulase- negative staphylococci following invasive neurosurgical procedures, particularly shunting procedures.
  • 11. PATHOPHYSIOLOGY • Bacteria are able to avoid phagocytosis by neutrophils and classic complement-mediated bactericidal activity because of the presence of a polysaccharide capsule multiply rapidly within CSF because of the absence of effective host immune defenses. • Normal CSF contains few white blood cells (WBCs) and relatively small amounts of complement proteins and immunoglobulins - prevents effective opsonization of bacteria, an essential prerequisite for bacterial phagocytosis by neutrophils. • Phagocytosis of bacteria is further impaired by the fluid nature of CSF, which is less conducive to phagocytosis than a solid tissue substrate.
  • 12.
  • 13. CLINICAL PRESENTATION • Classic clinical triad of meningitis is fever, headache, and nuchal rigidity, but the classic triad may not be present. • A decreased level of consciousness (>75%) • Nausea, vomitting, photophobia • Seizures (20–40%) • Focal seizures are usually due to focal arterial ischemia or infarction, cortical venous thrombosis with hemorrhage, or focal edema. • Generalized seizure activity and status epilepticus may be due to hyponatremia, cerebral anoxia, or, less commonly, the toxic effects of antimicrobial agents such as high-dose penicillin.
  • 14.
  • 15. • The CSF LA test has a specificity of 95–100% for S. pneumoniae and N. meningitidis. • Sensitivity of the CSF LA test is only 70–100% for detection of S. pneumoniae and 33–70% for detection of N. meningitidis antigens, so a negative test does not exclude infection by these organisms. • Limulus amebocyte lysate assay has a specificity of 85–100% and a sensitivity approaching 100%.
  • 16. Relationship between Cerebrospinal Fluid Glucose and Serum Glucose N Engl J Med 2012; 366:576-578February 9, 2012DOI: 10.1056/NEJMc1111080 • Bacterial meningitis typically have low levels of CSF glucose because of glycolysis by both white cells and the pathogen and impaired CSF glucose transport. • Level of CSF glucose is typically interpreted in relation to that of serum glucose, since glucose passes across the blood–brain barrier. Standard reference texts cite the normal ratio of CSF to serum glucose as 0.6,4 although this ratio has not been rigorously investigated. • Specifically, the normal level of CSF glucose should be approximately 60% of the level of serum glucose.
  • 17. EMPIRICAL ANTIMICROBIAL TREATMENT • Goal is to begin antimicrobial therapy within 60 minutes of patient’s arrival in the emergency room. • S. pneumoniae and N. meningitidis are the most common etiologic organisms of community-acquired bacterial meningitis.
  • 18. • Due to the emergence of penicillin- and cephalosporin-resistant S. pneumoniae, empirical therapy of community-acquired suspected bacterial meningitis in children and adults should include a combination of 1. Dexamethasone 2. Third- or fourth-generation cephalosporin (e.g., ceftriaxone, cefotaxime, or cefepime) 3. Vancomycin 4. Acyclovir, as HSV encephalitis is the leading disease in the differential diagnosis 5. Doxycycline during tick season in endemic area
  • 19. • Ceftriaxone or cefotaxime provide good coverage for - susceptible S. pneumoniae - group B streptococci - H. influenzae Adequate coverage for N. meningitidis • Cefepime is a broad-spectrum fourth-generation cephalosporin - in vitro activity similar to that of cefotaxime or ceftriaxone against S. pneumoniae and N. meningitidis -greater activity against Enterobacter species and Pseudomonas aeruginosa
  • 20. • Ampicillin should be added to the empirical regimen for coverage of L. monocytogenes in - individuals <3 months of age - adults >55 - with suspected impaired cell-mediated immunity because of chronic illness, organ transplantation, pregnancy, malignancy, or immunosuppressive therapy • Metronidazole is added to the empirical regimen to cover gram-negative anaerobes in patients with otitis, sinusitis, or mastoiditis.
  • 21. • In hospital-acquired meningitis, and particularly meningitis following neurosurgical procedures, staphylococci and gram- negative organisms including P. aeruginosa are the most common etiologic organisms. • Empirical therapy – - combination of vancomycin and ceftazidime, cefepime, or meropenem. - Ceftazidime, cefepime, or meropenem should be substituted for ceftriaxone or cefotaxime in neurosurgical patients and in neutropenic patients, as ceftriaxone and cefotaxime do not provide adequate activity against CNS infection with P. aeruginosa. - Meropenem is a carbapenem antibiotic that is highly active in vitro against L. monocytogenes, has been demonstrated to be effective in cases of meningitis caused by P. aeruginosa, and shows good activity against penicillin-resistant pneumococci.
  • 22.
  • 23. Specific Antimicrobial Therapy • Pneumococcal Meningitis - cephalosporin (ceftriaxone, cefotaxime, or cefepime) and vancomycin - Rifampin can be added to vancomycin for its synergistic effect but is inadequate as monotherapy because resistance develops rapidly when it is used alone. -2-week course of intravenous antimicrobial therapy is recommended. - Repeat LP performed 24–36 h after the initiation of antimicrobial therapy to document sterilization of the CSF. - Failure to sterilize the CSF after 24–36 h of antibiotic therapy should be considered presumptive evidence of antibiotic resistance. Patients may benefit from the addition of intraventricular vancomycin.
  • 24. • Meningococcal Meningitis - Penicillin G remains the antibiotic of choice for susceptible strains. - Ceftriaxone and cefotaxime provide adequate empirical coverage. - Isolates of N. meningitidis with moderate resistance to penicillin have still been successfully treated with penicillin. - A 7-day course of intravenous antibiotic therapy is adequate for uncomplicated meningococcal meningitis.
  • 25. Chemoprophylaxis for the close contacts • Close contacts are defined as those individuals who have had contact with oropharyngeal secretions, either through kissing or by sharing toys, beverages, or cigarettes. • 2-day regimen of rifampin (600 mg every 12 h for 2 days in adults and 10 mg/kg every 12 h for 2 days in children >1 year). Rifampin is not recommended in pregnant women. • Alternatively, adults can be treated with one dose of azithromycin (500 mg), or one intramuscular dose of ceftriaxone (250 mg).
  • 26. • Listeria Meningitis - Ampicillin for at least 3 weeks. - Gentamicin is added in critically ill patients (2 mg/kg loading dose, then 7.5 mg/kg per day given every 8 h). - Trimethoprim (10–20 mg/kg per day) and sulfamethoxazole (50–100 mg/kg per day) given every 6 h may provide an alternative in penicillin- allergic patients.
  • 27. • Staphylococcal Meningitis -Susceptible strains of S. aureus or coagulase- negative staphylococci is treated with nafcillin. -Vancomycin is the drug of choice for methicillin- resistant staphylococci and for patients allergic to penicillin. -If the CSF is not sterilized after 48 h of intravenous vancomycin therapy, then either intraventricular or intrathecal vancomycin, 20 mg once daily, can be added.
  • 28. • Gram-Negative Bacillary Meningitis - The third-generation cephalosporins— cefotaxime, ceftriaxone, and ceftazidime, with the exception of meningitis due to P. aeruginosa, which should be treated with ceftazidime, cefepime, or meropenem - 3-week course of intravenous antibiotic therapy is recommended
  • 29.
  • 30. Adjunctive Therapy • The release of bacterial cell-wall components by bactericidal antibiotics inflammatory cytokines IL-1 and TNF- in the subarachnoid space. • Dexamethasone - inhibits the synthesis of IL-1 and TNF - decreases CSF outflow resistance - stabilizes the blood-brain barrier
  • 31. • The results of clinical trials of dexamethasone therapy in children, predominantly with meningitis due to H. influenzae and S. pneumoniae, have demonstrated its efficacy in decreasing meningeal inflammation and incidence of sensorineural hearing loss. • A prospective European trial of adjunctive therapy for acute bacterial meningitis in 301 adults found that dexamethasone reduced the number of unfavorable outcomes (15 vs. 25%, p = .03) including death (7 vs. 15%, p = .04) • Dexamethasone (10 mg intravenously) was administered 15–20 min before the first dose of an antimicrobial agent, and the same dose was repeated every 6 h for 4 days.
  • 32. • Therapy with dexamethasone should ideally be started 20 min before, or not later than concurrent with, the first dose of antibiotics. • It is unlikely to be of significant benefit if started >6 h after antimicrobial therapy has been initiated. • Dexamethasone may decrease the penetration of vancomycin into CSF. • The rationale for giving dexamethasone 20 min before antibiotic therapy is that dexamethasone inhibits the production of TNF- by macrophages and microglia only if it is administered before these cells are activated by endotoxin. Dexamethasone does not alter TNF- production once it has been induced.
  • 33. • In experimental models of meningitis, dexamethasone therapy increased hippocampal cell injury and reduced learning capacity. This has not been the case in clinical series. • . Three large randomized trials in low-income countries (sub-Saharan Africa, Southeast Asia) failed to show benefit in subgroups of patients. - Attributed to late presentation to the hospital with more advanced disease, antibiotic pretreatment, malnutrition, infection with HIV. - The results of these clinical trials suggest that patients in sub-Saharan Africa and those in low-income countries with negative CSF Gram's stain and culture should not be treated with dexamethasone.
  • 34. VIRAL MENINGITIS • Headache, fever, and signs of meningeal irritation. • Frontal or retroorbital pain, photophobia and pain on moving the eyes. • Constitutional signs can include malaise, myalgia, anorexia, nausea and vomiting, abdominal pain, and/or diarrhea.
  • 35. Etiology • Enteroviruses (including echoviruses and coxsackieviruses) • HSV type 2 (HSV-2) • HIV • arboviruses Approximately two-thirds of culture- negative cases of "aseptic" meningitis have a specific viral etiology identified by CSF PCR testing.
  • 36. Laboratory Diagnosis CSF Examination - lymphocytic pleocytosis (25–500 cells/L) - normal or slightly elevated protein concentration] - normal glucose concentration - Organisms are not seen on Gram's stain of CSF. - Rarely, PMNs may predominate in the first 48 h of illness, especially with infections due to echovirus 9, West Nile virus, eastern equine encephalitis (EEE) virus, or mumps. - The CSF glucose concentration may be decreased in 10–30% of cases due to mumps or LCMV. As a rule, a lymphocytic pleocytosis with a low glucose concentration should suggest fungal or tuberculous meningitis, Listeria meningoencephalitis, or noninfectious disorders (e.g., sarcoid, neoplastic meningitis).
  • 37. Polymerase Chain Reaction Amplification of Viral Nucleic Acid - In both enteroviral and HSV infections of the CNS, PCR has become the diagnostic procedure of choice. - HSV PCR is also an important diagnostic test in patients with recurrent episodes of "aseptic" meningitis, many of whom have amplifiable HSV DNA in CSF despite negative viral cultures. - CSF PCR tests are available for WNV but are not as sensitive as detection of WNV-specific CSF IgM. - PCR is also useful in the diagnosis of CNS infection caused by Mycoplasma pneumoniae, which can mimic viral meningitis and encephalitis.
  • 38. Viral Culture • The sensitivity of CSF cultures, in contrast to its utility in bacterial infections, is generally poor. Serologic Studies • For some viruses, including many arboviruses such as WNV, serologic studies remain a crucial diagnostic tool. • Less useful for viruses with high seroprevalence rates in the general population such as HSV, VZV, CMV, and EBV. • CSF oligoclonal gamma globulin bands occur in association with a number of viral infections,also occur commonly in certain noninfectious neurologic diseases (e.g., multiple sclerosis) and nonviral infections (e.g., neurosyphilis, Lyme neuroborreliosis).
  • 39. TREATMENT • Symptomatic Rx - analgesics, antipyretics, and antiemetics. Fluid and electrolyte status should be monitored. • Oral or intravenous acyclovir – HSV-1 or -2 severe EBV or VZV infection • Seriously ill patients – intravenous acyclovir (15–30 mg/kg per day in three divided doses), which can be followed by an oral drug such as acyclovir (800 mg, five times daily), famciclovir (500 mg tid), or valacyclovir (1000 mg tid) for a total course of 7–14 days. • Patients who are less ill can be treated with oral drugs alone.
  • 40. SUBACUTE MENINGITIS • Unrelenting headache, stiff neck, low-grade fever, and lethargy for days to several weeks before they present for evaluation. • Cranial nerve abnormalities and night sweats may be present. ETIOLOGY • M. Tuberculosis • C. neoformans • C. Immitis • T. Pallidum
  • 41. Laboratory Diagnosis CSF : (1) elevated opening pressure (2) lymphocytic pleocytosis (10–500 cells/L) (3) elevated protein concentration 4) decreased glucose • Positive AFB smears - 10–40% of cases of tuberculous meningitis in adults. • Cultures of CSF for TB are positive in 50% of adults. Culture remains the gold standard to make the diagnosis of tuberculous meningitis. • PCR for the detection of M. tuberculosis DNA - sensitivity and specificity on CSF have not been defined. • The Centers for Disease Control and Prevention recommend the use of nucleic acid amplification tests for the diagnosis of pulmonary tuberculosis.
  • 42. • CSF abnormalities in fungal meningitis are a mononuclear or lymphocytic pleocytosis, an increased protein concentration, and a decreased glucose concentration. • There may be eosinophils in the CSF in C. immitis meningitis. • The cryptococcal polysaccharide antigen test is a highly sensitive and specific test for cryptococcal meningitis. • The detection of the histoplasma polysaccharide antigen in CSF establishes the diagnosis of a fungal meningitis but is not specific for meningitis due to H. capsulatum. It may be falsely positive in coccidioidal meningitis.
  • 43. Empirical therapy of tuberculous meningitis • Isoniazid (300 mg/d), Rifampin (10 mg/kg per day), Pyrazinamide (30 mg/kg per day in divided doses), Ethambutol (15–25 mg/kg per day in divided doses), and pyridoxine (50 mg/d). • If the clinical response is good, pyrazinamide can be discontinued after 8 weeks and isoniazid and rifampin continued alone for the next 6–12 months. • A 6-month course of therapy is acceptable, but therapy should be prolonged for 9–12 months in patients who have an inadequate resolution of symptoms of meningitis or who have positive mycobacterial cultures of CSF during the course of therapy. • Dexamethasone therapy is recommended for HIV-negative patients with tuberculous meningitis. • The dose is 12–16 mg per day for 3 weeks, then tapered over 3 weeks.
  • 44. Meningitis due to C. neoformans in non-HIV, nontransplant patients • Induction therapy - amphotericin B (AmB) (0.7 mg/kg IV per day) plus flucytosine (100 mg/kg per day in four divided doses) for at least 4 weeks if CSF culture results are negative after 2 weeks of treatment. • Therapy should be extended for a total of 6 weeks in the patient with neurologic complications. • Consolidation therapy - fluconazole 400 mg per day for 8 weeks.
  • 45. Organ transplant recipients/ HIV infected : • liposomal AmB (3–4 mg/kg per day) or AmB lipid complex (ABLC) 5 mg/kg per day plus flucytosine (100 mg/kg per day in four divided doses) for at least 2 weeks or until CSF culture is sterile. • Followed by an 8- to 10-week course of fluconazole [400–800 mg/d (6–12 mg/kg) PO]. • If the CSF culture is sterile after 10 weeks of acute therapy, the dose of fluconazole is decreased to 200 mg/d for 6 months to a year. • HIV-infected patients may require indefinite maintenance therapy with fluconazole 200 mg/day.