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AUTHOR AND EDITOR INFORMATION

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Author: Niranjan N Singh, MD, DNB, Fellow in Neurophysiology, Department of Neurology, St Louis University School of Medicine

Niranjan N Singh is a member of the following medical societies: American Academy of Neurology

Coauthor(s): Florian P Thomas, MD, MA, PhD, Drmed, Director, Spinal Cord Injury Unit, St Louis Veterans Affairs Medical Center; Director, National MS Society Multiple Sclerosis Center; Associate Program Director, Professor, Department of Neurology and Psychiatry, Associate Professor, Institute for Molecular Virology, and Department of Molecular Microbiology and Immunology, St Louis University; Mandeep Garewal, MD, Staff Physician, Department of Neurology, Saint Louis University School of Medicine; Sofia Yahya, MD, Staff Physician, Department of Psychiatry, Barnes-Jewish Hospital, Washington University School of Medicine

Editors: William J Nowack, MD, Associate Professor, Department of Neurology, Epilepsy Center, University of Kansas Medical Center; Francisco Talavera, PharmD, PhD, Senior Pharmacy Editor, eMedicine; Glenn Lopate, MD, Associate Professor, Department of Neurology, Division of Neuromuscular Diseases, Washington University School of Medicine; Chief of Neurology, St Louis ConnectCare, Consulting Staff, Barnes Jewish Hospital; Selim R Benbadis, MD, Professor, Director of Comprehensive Epilepsy Program, Departments of Neurology and Neurosurgery, University of South Florida School of Medicine, Tampa General Hospital; Nicholas Y Lorenzo, MD, Chief Editor, eMedicine Neurology; Consulting Staff, Neurology Specialists and Consultants

Author and Editor Disclosure

Synonyms and related keywords: AIDP, CIDP, GBS, Guillain-Barré syndrome, Landry-Guillain-Barré syndrome, Landry-Guillain-Barré-Strohl syndrome, acquired immunodeficiency syndrome, AIDS

INTRODUCTION

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Background

HIV infection is now an important cause of inflammatory demyelinating neuropathies. Exclude HIV infection in any patient who presents with these conditions. The history, physical examination, and course resemble those of HIV-seronegative patients. In two case series, up to 30% of patients presenting with Guillian-Barré syndrome (GBS) were found to be HIV positive.

Pathophysiology

While many of the clinical manifestations of HIV infection are caused by immune deficiency, others, such as thrombocytopenic purpura, are a manifestation of the general state of immune activation evidenced by T-cell activation and hypergammaglobulinemia, which can result in autoimmunity.

Similar mechanisms are responsible for the increased incidence of acute inflammatory demyelinating polyradiculoneuropathy (AIDP) and chronic inflammatory demyelinating polyradiculoneuropathy (CIDP) compared with the HIV-seronegative population. Several in vitro studies have shown that the binding of HIV envelope protein Gp120 to chemokine receptors leads to activation of caspase pathway and axonal degeneration. Perineuronal Schwann cells may have a neuroprotective role.

Frequency

United States

Two studies demonstrate that inflammatory demyelinating neuropathies are diagnosed in one third of HIV-seropositive patients referred for peripheral nerve diseases.

While CIDP was much more frequent than AIDP in two European and North American reports, the converse was true in a larger series of African patients: 16 AIDP but no CIDP patients were found.


CLINICAL

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History

While AIDP presents most often at the time of seroconversion, it also can occur in late AIDS. CIDP can occur at any phase of HIV disease.

AIDP progresses over days to less than 4 weeks.

CIDP has a chronic progression for more than 2 months or a relapsing and/or remitting course.

HIV-GBS has been associated with more frequent recurrent episodes or the development of CIDP as compared to HIV-seronegative GBS.

Characteristic features include the following:

  • Distal and proximal weakness
  • Mild sensory complaints and pain
  • Respiratory paralysis in AIDP
  • Cranial neuropathy (VII, X, XII) in AIDP and CIDP

Physical

AIDP and CIDP present with an acute, subacute, chronic, or relapsing and/or remitting course, with the following signs:

  • Distal and proximal weakness
  • Mildly impaired sensation
  • Autonomic dysfunction with cardiac arrhythmia, urinary retention, and blood pressure instability
  • Hyporeflexia or areflexia


DIFFERENTIALS

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Acute Inflammatory Demyelinating Polyradiculoneuropathy
Cervical Spondylosis: Diagnosis and Management
Chronic Inflammatory Demyelinating Polyradiculoneuropathy
Diabetic Neuropathy
HIV-1 Associated Distal Painful Sensorimotor Polyneuropathy
HIV-1 Associated Multiple Mononeuropathies
HIV-1 Associated Progressive Polyradiculopathy
Median Neuropathy
Neuropathy of Leprosy
Peroneal Mononeuropathy
Polyarteritis Nodosa
Radial Mononeuropathy
Sarcoidosis and Neuropathy
Toxic Neuropathy
Ulnar Neuropathy

Other Problems to be Considered

Acute or subacute neuropathies of other causes
Hereditary Motor and Sensory Neuropathies
Lumbosacral disk syndromes
Lumbosacral spondylosis
Paraneoplastic neuropathy
Paraneoplastic sensory neuropathy
Paraproteinemic Neuropathy


WORKUP

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Lab Studies

  • Cerebrospinal fluid
    • In HIV-GBS, CSF may demonstrate a mild lymphocytic pleocytosis (10-50 cells/µL), which helps differentiate it from GBS in HIV-seronegative patients. Similarly, the presence of pleocytosis in a patient with AIDP warrants consideration of underlying HIV disease.
    • Significantly elevated protein is another characteristic finding.
  • Electromyography nerve conduction studies (EMG/NCS) - Findings consistent with a primarily demyelinating process, often with secondary axonal degeneration
    • Reduced motor nerve conduction velocity
    • Conduction block or temporal dispersion
    • Prolonged F-wave latencies
    • Prolonged distal latencies
    • Variable reduction of compound muscle action potential amplitudes
    • Variable spontaneous activity due to axonal degeneration

Histologic Findings

Segmental demyelination, mononuclear perivascular infiltration in the endoneurium, perineurial edema, variable Wallerian degeneration, viral particles, and RNA usually are not present.


TREATMENT

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Medical Care

  • Treatment is similar to that of HIV-seronegative patients. Intravenous immunoglobulin (IVIG) and plasmapheresis (plasma exchange) are preferred to immunosuppression. In patients with CIDP, oral prednisone can also be used until clinical improvement, and then it can be titrated off.
    • During a 7- to 10-day period, 4-5 plasmapheresis procedures may be performed as described in standard protocols. Potential complications include autonomic instability, hypercalcemia, and bleeding caused by depletion of clotting factors.
    • Decide among IVIG, plasmapheresis, and steroids on an individual basis. The cost of IVIG, the invasive nature of plasmapheresis, and the long-term side effects of steroids are important points to consider when making a selection.
  • In advanced HIV disease, with CD4+ count of less than 100 cells/µL, opportunistic infections such as CMV may need to be investigated and empiric therapy instituted.


MEDICATION

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The goal is to diminish the general state of immune activation as evidenced by T-cell activation and hypergammaglobulinemia, which may be responsible for autoimmunity.

Drug Category: Blood products

IVIG is an effective treatment of autoimmune neuropathies in general. It reduces the duration of hospitalization and the need for mechanical ventilation.

Drug NameIntravenous immunoglobulin (Gammagard, Gammar-P, Sandoglobulin)
DescriptionFeatures that may be relevant to its efficacy include neutralization of circulating myelin antibodies through anti-idiotypic antibodies; downregulation of proinflammatory cytokines, including IFN-gamma; blockade of Fc receptors on macrophages; suppression of inducer T and B cells and augmentation of suppressor T cells; blockade of the complement cascade; promotion of remyelination; 10% increase in CSF IgG.
Adult Dose2 g/kg IV over 2-5 d
Pediatric DoseAdminister as in adults
ContraindicationsDocumented hypersensitivity; IgA deficiency; anti-IgE/IgG antibodies
InteractionsNone reported
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsConsider checking serum IgA before IVIG and using IgA-depleted IVIG (G-Gard-SD) if indicated; IVIG may increase serum viscosity and thromboembolic events; the following adverse effects have been reported: migraine attacks; 10% increased risk of aseptic meningitis; increased risk of urticaria, pruritus, or petechiae 2-5 d postinfusion, possibly lasting up to 1 month; increased risk of renal tubular necrosis in older patients, patients with diabetes, volume-depleted patients, and patients with preexisting kidney disease; IVIG can lead to elevated antiviral or antibacterial antibody titers for 1 mo, 6-fold increased ESR for 2-3 wk, and apparent hyponatremia

Drug Category: Glucocorticoids

These agents modify the body's immune response to diverse stimuli. Likely mechanisms of action include inhibition of synthesis and/or secretion of TNF-alpha, IL-6, IL-2, and IFN-gamma and modulation of serum and leukocyte-bound levels of cell adhesion molecules.

Drug NamePrednisone (Deltasone, Orasone, Sterapred)
DescriptionIndicated in treatment of CIDP but not AIDP (GBS).
Adult Dose60-100 mg PO qam for several mo or until clinical improvement; taper slowly to qod
Pediatric Dose4-5 mg/m2/d for several months or until clinical improvement; taper slowly to qod
Alternative dose: 1-2 mg/kg PO qd for several mo or until clinical improvement; taper slowly to qod
ContraindicationsDocumented hypersensitivity, caution in patients with opportunistic infections
InteractionsClearance may decrease when used with estrogens; when used with digoxin, digitalis toxicity may increase secondary to hypokalemia; phenobarbital, phenytoin, and rifampin also may increase metabolism of glucocorticoids and may necessitate a dose increase; monitor for hypokalemia when administered concurrently with diuretics
PregnancyB - Usually safe but benefits must outweigh the risks.
PrecautionsCaution in patients with hyperthyroidism, cirrhosis, nonspecific ulcerative colitis, osteoporosis, peptic ulcer, diabetes, and myasthenia gravis; patients may develop hyperglycemia, edema, osteonecrosis, peptic ulcer disease, hypokalemia, osteoporosis, euphoria, acne, psychosis, growth suppression, myalgia, myopathy, infections, glaucoma, hirsutism, and facial plethora; if steroids are withdrawn abruptly, patients may develop adrenal crisis


FOLLOW-UP

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Prognosis

  • The prognosis of HIV-1 associated AIDP and CIDP is similar to that of HIV-seronegative varieties discussed in separate eMedicine articles (Acute Inflammatory Demyelinating Polyradiculoneuropathy, Chronic Inflammatory Demyelinating Polyradiculoneuropathy).
  • In one study comparing GBS in HIV-seropositive patients to HIV-seronegative patients in the ICU requiring ventilation, no significant difference existed between the two groups in days spent in the ICU or days ventilated, particularly if patient with HIV-associated GBS had a CD4 T-lymphocyte count greater than 200 X 106 cells/L at admission.

Patient Education


MISCELLANEOUS

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Medical/Legal Pitfalls

  • Failure to ascertain HIV status in patients carrying these diagnoses. As mentioned, AIDP can occur at HIV seroconversion in what appears to be an otherwise healthy individual.


REFERENCES

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  • Cornblath DR, McArthur JC, Kennedy PG, et al. Inflammatory demyelinating peripheral neuropathies associated with human T-cell lymphotropic virus type III infection. Ann Neurol. Jan 1987;21(1):32-40. [Medline].
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  • Leger JM, Bouche P, Bolgert F, et al. The spectrum of polyneuropathies in patients infected with HIV. J Neurol Neurosurg Psychiatry. Dec 1989;52(12):1369-74. [Medline].
  • Said G, Saimont AG, Lacroix C. Neurological Complications of HIV and AIDS. Philadelphia: WB Saunders;1998.
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  • Simpson DM, Olney RK. Peripheral neuropathies associated with human immunodeficiency virus infection. Neurol Clin. Aug 1992;10(3):685-711. [Medline].
  • Thornton CA, Latif AS, Emmanuel JC. Guillain-Barre syndrome associated with human immunodeficiency virus infection in Zimbabwe. Neurology. Jun 1991;41(6):812-5. [Medline].
  • Verma A. Epidemiology and clinical features of HIV-1 associated neuropathies. J Peripher Nerv Syst. Mar 2001;6(1):8-13. [Medline].
  • Verma S, Micsa E, Estanislao L, Simpson D. Neuromuscular complications in HIV. Curr Neurol Neurosci Rep. Jan 2004;4(1):62-7. [Medline].
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HIV-1 Associated Acute/Chronic Inflammatory Demyelinating Polyneuropathy excerpt

Article Last Updated: Mar 13, 2007