Autoimmune lymphoproliferative syndrome: Difference between revisions
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==Introduction== | ==Introduction== | ||
Autoimmune Lymphoproliferative Syndrome (ALPS) is a rare disorder of abnormal [[lymphocyte]] survival caused by defective [[Fas]] mediated [[apoptosis]]. Normally, after infectious insult, the immune system down-regulates by increasing Fas expression on activated B and T lymphocytes and Fas-ligand on activated T lymphocytes. Fas and Fas-ligand interact to trigger the caspase cascade, leading to cell apoptosis. Patients with ALPS have a defect in this apoptotic pathway, leading to chronic non-malignant lymphoproliferation, autoimmune disease, and secondary cancers. | Autoimmune Lymphoproliferative Syndrome (ALPS) is a rare disorder of abnormal [[lymphocyte]] survival caused by defective [[Fas]] mediated [[apoptosis]]. Normally, after infectious insult, the immune system down-regulates by increasing Fas expression on activated B and T lymphocytes and Fas-ligand on activated T lymphocytes. Fas and Fas-ligand interact to trigger the caspase cascade, leading to cell apoptosis. Patients with ALPS have a defect in this apoptotic pathway, leading to chronic non-malignant lymphoproliferation, autoimmune disease, and secondary cancers.<ref name="pmid19930184">{{cite journal| author=Teachey DT, Seif AE, Grupp SA| title=Advances in the management and understanding of autoimmune lymphoproliferative syndrome (ALPS). | journal=Br J Haematol | year= 2010 | volume= 148 | issue= 2 | pages= 205-16 | pmid=19930184 | doi=10.1111/j.1365-2141.2009.07991.x | pmc=PMC2929682 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19930184 }} </ref> | ||
==Clinical Manifestations== | ==Clinical Manifestations== | ||
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* Lymphoproliferation tends to present at a young age (median 11.5 months) and may improve with age. | * Lymphoproliferation tends to present at a young age (median 11.5 months) and may improve with age. | ||
Autoimmune disease: The second most common clinical manifestation and one that most often requires treatment. | Autoimmune disease: The second most common clinical manifestation and one that most often requires treatment. | ||
* Autoimmune cytopenias: Most common. Can be mild to very severe. Can be intermittent or chronic. | * Autoimmune cytopenias: Most common. Can be mild to very severe. Can be intermittent or chronic.<ref name="pmid15542578">{{cite journal| author=Teachey DT, Manno CS, Axsom KM, Andrews T, Choi JK, Greenbaum BH et al.| title=Unmasking Evans syndrome: T-cell phenotype and apoptotic response reveal autoimmune lymphoproliferative syndrome (ALPS). | journal=Blood | year= 2005 | volume= 105 | issue= 6 | pages= 2443-8 | pmid=15542578 | doi=10.1182/blood-2004-09-3542 | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=15542578 }} </ref> | ||
** Autoimmune [[Hemolytic Anemia]] | ** Autoimmune [[Hemolytic Anemia]] | ||
** Autoimmune [[Neutropenia]] | ** Autoimmune [[Neutropenia]] | ||
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* Genetic mutations in ALPS causative genes (see below) | * Genetic mutations in ALPS causative genes (see below) | ||
* Biomarkers | * Biomarkers | ||
** Polyclonal [[hypergammaglobulinemia]] | ** Polyclonal [[hypergammaglobulinemia]]<ref name="pmid20068224">{{cite journal| author=Seif AE, Manno CS, Sheen C, Grupp SA, Teachey DT| title=Identifying autoimmune lymphoproliferative syndrome in children with Evans syndrome: a multi-institutional study. | journal=Blood | year= 2010 | volume= 115 | issue= 11 | pages= 2142-5 | pmid=20068224 | doi=10.1182/blood-2009-08-239525 | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=20068224 }} </ref> | ||
** Elevated serum FASL | ** Elevated serum FASL | ||
** Elevated plasma [[IL-10]] and/or IL-18 | ** Elevated plasma [[IL-10]] and/or IL-18 | ||
| Line 137: | Line 137: | ||
*** Consider PCP prophylaxis but usually not needed | *** Consider PCP prophylaxis but usually not needed | ||
** [[Sirolimus]] (rapamycin, rapamune) | ** [[Sirolimus]] (rapamycin, rapamune) | ||
*** mTOR ([[mammalian target of rapamycin]]) inhibitor | *** mTOR ([[mammalian target of rapamycin]]) inhibitor<ref name="pmid16757690">{{cite journal| author=Teachey DT, Obzut DA, Axsom K, Choi JK, Goldsmith KC, Hall J et al.| title=Rapamycin improves lymphoproliferative disease in murine autoimmune lymphoproliferative syndrome (ALPS). | journal=Blood | year= 2006 | volume= 108 | issue= 6 | pages= 1965-71 | pmid=16757690 | doi=10.1182/blood-2006-01-010124 | pmc=PMC1895548 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=16757690 }} </ref> | ||
*** Active in most patients | *** Active in most patients | ||
*** Second most studied agent in clinical trials | *** Second most studied agent in clinical trials | ||
*** Most patients have complete resolution of autoimmune disease (>90%) | *** Most patients have complete resolution of autoimmune disease (>90%)<ref name="pmid19208097">{{cite journal| author=Teachey DT, Greiner R, Seif A, Attiyeh E, Bleesing J, Choi J et al.| title=Treatment with sirolimus results in complete responses in patients with autoimmune lymphoproliferative syndrome. | journal=Br J Haematol | year= 2009 | volume= 145 | issue= 1 | pages= 101-6 | pmid=19208097 | doi=10.1111/j.1365-2141.2009.07595.x | pmc=PMC2819393 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19208097 }} </ref> | ||
*** Most patients have complete resolution of lymphoproliferation, including lymphadenopathy and splenomegaly (>90%) | *** Most patients have complete resolution of lymphoproliferation, including lymphadenopathy and splenomegaly (>90%) | ||
*** Some patients have near complete response (disease flares with viral illness) | *** Some patients have near complete response (disease flares with viral illness) | ||
| Line 146: | Line 146: | ||
*** Most patients have elimination of peripheral blood DNTs | *** Most patients have elimination of peripheral blood DNTs | ||
*** mTOR/Akt/PI3K pathway may be activated in abnormal ALPS cells: mTOR inhibitors may be targeted therapy | *** mTOR/Akt/PI3K pathway may be activated in abnormal ALPS cells: mTOR inhibitors may be targeted therapy | ||
*** May not be as immune suppressive in normal lymphocytes as other agents. Some patients have had improvement in immune function with transition from cellcept to rapamycin | *** May not be as immune suppressive in normal lymphocytes as other agents. Some patients have had improvement in immune function with transition from cellcept to rapamycin<ref name="pmid21475130">{{cite journal| author=Teachey DT| title=Autoimmune lymphoproliferative syndrome: new approaches to diagnosis and management. | journal=Clin Adv Hematol Oncol | year= 2011 | volume= 9 | issue= 3 | pages= 233-5 | pmid=21475130 | doi= | pmc= | url= }} </ref> | ||
*** Not reported to cause hypogammaglobulinemia | *** Not reported to cause hypogammaglobulinemia | ||
*** Hypothetically, may have lower risk of secondary cancers as opposed to other immune suppressants | *** Hypothetically, may have lower risk of secondary cancers as opposed to other immune suppressants | ||
Revision as of 17:25, 14 October 2011
| Autoimmune lymphoproliferative syndrome | |
| OMIM | 601859 603909 |
|---|---|
| DiseasesDB | 33425 Template:DiseasesDB2 |
Editor-In-Chief: David Teachey, MD [1]
Please Take Over This Page and Apply to be Editor-In-Chief for this topic: There can be one or more than one Editor-In-Chief. You may also apply to be an Associate Editor-In-Chief of one of the subtopics below. Please mail us [2] to indicate your interest in serving either as an Editor-In-Chief of the entire topic or as an Associate Editor-In-Chief for a subtopic. Please be sure to attach your CV and or biographical sketch.
Autoimmune lymphoproliferative syndrome is a form of lymphoproliferative disorder. It affects lymphocyte apoptosis.[1]
Introduction
Autoimmune Lymphoproliferative Syndrome (ALPS) is a rare disorder of abnormal lymphocyte survival caused by defective Fas mediated apoptosis. Normally, after infectious insult, the immune system down-regulates by increasing Fas expression on activated B and T lymphocytes and Fas-ligand on activated T lymphocytes. Fas and Fas-ligand interact to trigger the caspase cascade, leading to cell apoptosis. Patients with ALPS have a defect in this apoptotic pathway, leading to chronic non-malignant lymphoproliferation, autoimmune disease, and secondary cancers.[2]
Clinical Manifestations
Lymphoproliferation: The most common clinical manifestation of ALPS is lymphoproliferation, affecting 100% of patients.
- Lymphadenopathy: >90% of patients present with chronic non-malignant lymphadenopathy. It can be mild to severe, affecting multiple nodal groups. Most commonly presents with massive non-painful hard cervical lymphadenopathy
- Splenomegaly: >80% of patients present with clinically identifiable splenomegaly. It can be massive.
- Hepatomegaly: 30-40% of patients have enlarged livers.
- Lymphoproliferation tends to present at a young age (median 11.5 months) and may improve with age.
Autoimmune disease: The second most common clinical manifestation and one that most often requires treatment.
- Autoimmune cytopenias: Most common. Can be mild to very severe. Can be intermittent or chronic.[3]
- Autoimmune Hemolytic Anemia
- Autoimmune Neutropenia
- Autoimmune Thrombocytopenia
- Other: Can affect any organ system similar to systemic lupus erythematosis (most rare affecting <5% of patients)
- Nervous: Autoimmune cerebellar ataxia; Guillain-Barre; Transverse myelitis
- GI: Autoimmune esophagitis, gastritis, colitis, hepatitis, pancreatitis
- Derm: Urticaria
- Pulmonary: Bronchiolitis obliterans
- Renal: Autoimmune glomerulonephritis, nephrotic syndrome
- Cancer: Secondary neoplasms affect approximately 10% of patients. True prevalence unknown as <20 reported cases of cancer. Most common EBER+ Non-Hodgkin's and Hodgkin's lymphoma
- Unaffected family members with genetic mutations are also at increased risk of developing cancer
Laboratory Manifestations
- Elevated peripheral blood Double Negative T cells (DNTs)
- Required for diagnosis
- Immunophenotype: CD3+/CD4-/CD8-/TCRalpha/beta+
- Measured by flow cytometry: Normal values <2.5% total T cells; <1% of total lymphocytes in peripheral blood
- Marked elevations >5% virtually pathognomic for ALPS
- Mild elevations also found in other autoimmune diseases
- Thought to be cytotoxic T lymphocytes that have lost CD8 expression
- ?Unknown if driver of disease or epiphenomenon
- May be falsely elevated in setting of lymphopenia or falsely decreased with immunosuppressive treatment
- Defective in vitro Fas mediated apoptosis
- Required for diagnosis under old definition. Now can be used to make diagnosis; however, not required to make diagnosis.
- Time and labor intensive assay.
- T cells from patient and normal control supported in culture for >10 days with mitogen stimulation and IL-2 expansion and then exposed to anti-Fas IgM monoclonal antibody
- ALPS patient T cells: Do not die with anti-Fas monoclonal antibody exposure. Normal T cells from unaffected patient do.
- False negative in somatic Fas variant ALPS and FasL variant ALPS
- Genetic mutations in ALPS causative genes (see below)
- Biomarkers
- Polyclonal hypergammaglobulinemia[4]
- Elevated serum FASL
- Elevated plasma IL-10 and/or IL-18
- Elevated plasma or serum vitamin B12
- Autoantibodies: Non-specific. Can have antibodies to blood cells (DAT, anti-neutrophil, anti-platelet). Also, can have positive ANA, RF, ANCA.
Classification
Old nomenclature:
- IA - Fas
- IB - Fas ligand
- IIA - Caspase 10
- IIB - Caspase 8
- III - unknown
- IV - Neuroblastoma RAS viral oncogene homolog
Revised nomenclature (2010)
- ALPS-FAS: Fas. Germline FAS mutations. 70% of patients
- ALPS-sFAS:Fas. Somatic FAS mutations in DNT compartment. 10% of patients
- ALPS-FASL: Fas ligand. Germline FASL mutations. 3 reported cases
- ALPS-CASP10: Caspase 10. Germline CASP10 mutation. 2% of patients
- ALPS-U: Undefined. 20% of patients
- CEDS: Caspase 8 deficiency state. No longer considered a subtype of ALPS but distinct disorder
- RALD: NRAS , KRAS. Somatic mutations in NRAS and KRAS in lympocyte comparment. No longer considered a subtype of ALPS but distinct disesase
Diagnostic Algorithm
Old criteria
- Required
- Chronic non-malignant lymphoproliferation
- Elevated peripheral blood DNTs
- Defective in vitro Fas mediated apoptosis
New criteria
- Required
- Chronic non-malignant lymphoproliferation (>6 months lymphadenopathy and/or splenomegaly)
- Elevated peripheral blood DNTs
- Accessory
- Primary Accessory
- Defective in vitro Fas mediated apoptosis
- Somatic or germline mutation in ALPS causative gene (FAS, FASL, CASP10)
- Secondary Accessory
- Elevated biomarkers
- Plasma sFASL >200pg/ml
- Plasma IL-10 >20pg/ml
- Plasma or serum vitamin B12 >1500ng/L
- Plasma IL-18 >500pg/ml
- Immunohistochemical findings on biopsy consistent with ALPS as determined by experienced hematopathologist
- Autoimmune cytopenias and polyclonal hypergammaglobulinemia
- Family history of ALPS or non-malignant lymphoproliferation
- Elevated biomarkers
- Primary Accessory
- Definitive diagnosis: Required plus one primary accessory criteria
- Probable diagnosis: Required plus one secondary accessory criteria
- Definitive and Probable ALPS should be TREATED THE SAME and patients counseled that they have ALPS if definitive or probable
Treatment
- Mostly commonly directed at autoimmune disease
- Maybe needed to treat bulky lymphoproliferation
- First line therapies
- Corticosteroids
- Very active but toxic with chronic use
- IVIgG
- Not as effective as in other immune cytopenia syndromes
- Corticosteroids
- Second line therapies
- Mycophenolate mofetil (cellcept)
- Inactivates inosine monophosphate
- Active in most patients
- Most studied medicine in clinical trials
- Some patients have complete resolution of autoimmune disease
- Many patients have partial responses
- Some patients relapse
- Does not affect lymphoproliferation or reduce DNTs
- Well-tolerated: Side effects: Diarrhea, neutropenia
- Does not require therapeutic drug monitoring
- No drug-drug interactions
- Can cause hypogammaglobulinemia (transient) requiring IVIgG replacement
- Consider PCP prophylaxis but usually not needed
- Sirolimus (rapamycin, rapamune)
- mTOR (mammalian target of rapamycin) inhibitor[5]
- Active in most patients
- Second most studied agent in clinical trials
- Most patients have complete resolution of autoimmune disease (>90%)[6]
- Most patients have complete resolution of lymphoproliferation, including lymphadenopathy and splenomegaly (>90%)
- Some patients have near complete response (disease flares with viral illness)
- A few patients have had partial responses (most commonly patient with non-cytopenia autoimmune disease)
- Most patients have elimination of peripheral blood DNTs
- mTOR/Akt/PI3K pathway may be activated in abnormal ALPS cells: mTOR inhibitors may be targeted therapy
- May not be as immune suppressive in normal lymphocytes as other agents. Some patients have had improvement in immune function with transition from cellcept to rapamycin[7]
- Not reported to cause hypogammaglobulinemia
- Hypothetically, may have lower risk of secondary cancers as opposed to other immune suppressants
- Always a risk with any agent in pre-cancerous syndrome as immune suppression can decreased tumor immunosurvellence
- mTOR inhibitors active against lymphomas, especially EBV+ lymphomas. Thus, THEORETICALLY could eliminate malignant clones.
- Requires therapeutic drug monitoring
- Goal serum trough 5-15ng/ml
- Drug-drug interactions
- Well tolerated: Side effects: mucositis, diarrhea, hyperlipidemia, delayed wound healing
- Consider PCP prophylaxis but usually not needed
- Other agents:
- Fansidar, mercaptopurine: More commonly used in Europe. Good ancedotal data
- Rituximab: AVOID. Can cause life long hypogammaglobulinemia
- Splenectomy: AVOID. >30% risk of pneumococcal sepsis even with vaccination and antibiotic prophylaxis
- Mycophenolate mofetil (cellcept)
References
- ↑ Fleisher TA (2008). "The autoimmune lymphoproliferative syndrome: an experiment of nature involving lymphocyte apoptosis". Immunol. Res. 40 (1): 87–92. doi:10.1007/s12026-007-8001-1. PMID 18193364.
- ↑ Teachey DT, Seif AE, Grupp SA (2010). "Advances in the management and understanding of autoimmune lymphoproliferative syndrome (ALPS)". Br J Haematol. 148 (2): 205–16. doi:10.1111/j.1365-2141.2009.07991.x. PMC 2929682. PMID 19930184.
- ↑ Teachey DT, Manno CS, Axsom KM, Andrews T, Choi JK, Greenbaum BH; et al. (2005). "Unmasking Evans syndrome: T-cell phenotype and apoptotic response reveal autoimmune lymphoproliferative syndrome (ALPS)". Blood. 105 (6): 2443–8. doi:10.1182/blood-2004-09-3542. PMID 15542578.
- ↑ Seif AE, Manno CS, Sheen C, Grupp SA, Teachey DT (2010). "Identifying autoimmune lymphoproliferative syndrome in children with Evans syndrome: a multi-institutional study". Blood. 115 (11): 2142–5. doi:10.1182/blood-2009-08-239525. PMID 20068224.
- ↑ Teachey DT, Obzut DA, Axsom K, Choi JK, Goldsmith KC, Hall J; et al. (2006). "Rapamycin improves lymphoproliferative disease in murine autoimmune lymphoproliferative syndrome (ALPS)". Blood. 108 (6): 1965–71. doi:10.1182/blood-2006-01-010124. PMC 1895548. PMID 16757690.
- ↑ Teachey DT, Greiner R, Seif A, Attiyeh E, Bleesing J, Choi J; et al. (2009). "Treatment with sirolimus results in complete responses in patients with autoimmune lymphoproliferative syndrome". Br J Haematol. 145 (1): 101–6. doi:10.1111/j.1365-2141.2009.07595.x. PMC 2819393. PMID 19208097.
- ↑ Teachey DT (2011). "Autoimmune lymphoproliferative syndrome: new approaches to diagnosis and management". Clin Adv Hematol Oncol. 9 (3): 233–5. PMID 21475130.