PedAM

Pediatric Disease Annotations & Medicines


	churg-strauss syndrome

Disease ID	1128
Disease	churg-strauss syndrome
Definition	Widespread necrotizing angiitis with granulomas. Pulmonary involvement is frequent. Asthma or other respiratory infection may precede evidence of vasculitis. Eosinophilia and lung involvement differentiate this disease from POLYARTERITIS NODOSA.
Synonym	allergic angiitides allergic angiitides, granulomatous allergic angiitis allergic angiitis and granulomatosis allergic angiitis, granulomatous allergic granulomatoses allergic granulomatosis allergic granulomatosis angiitis allergic granulomatosis angiitis (disorder) allergic granulomatosis of churg-strauss allergic granulomatous and angiitis allergic granulomatous angiitides allergic granulomatous angiitis angiitides, allergic angiitides, allergic granulomatous angiitides, granulomatous allergic angiitis, allergic angiitis, allergic granulomatous angiitis, granulomatous allergic churg strauss churg strauss syndrome churg strauss vasculitis churg-strauss syndrome [disease/finding] churg-strauss vasculitis churg-strauss vasculitis (disorder) css - churg-strauss syndrome eosinophilic granulomatous vasculitides eosinophilic granulomatous vasculitis granulomatoses, allergic granulomatosis, allergic granulomatous allergic angiitides granulomatous allergic angiitis granulomatous angiitides, allergic granulomatous angiitis, allergic granulomatous vasculitides, eosinophilic granulomatous vasculitis, eosinophilic strauss churg strauss churg syndrome syndrome, churg-strauss vasculitides, eosinophilic granulomatous vasculitis, churg strauss vasculitis, churg-strauss vasculitis, eosinophilic granulomatous
DOID	DOID:3049
UMLS	C0008728
MeSH	D015267
SNOMED-CT	SNOMEDCT_US_2016_09_01:82275008
Comorbidity	UMLS \| Disease \| Sentences' Count(Total Sentences:58) C0442874 \| neuropathy \| 4 C0027059 \| myocarditis \| 4 C0152025 \| polyneuropathy \| 3 C0007785 \| cerebral infarct \| 3 C0007785 \| cerebral infarction \| 3 C0007785 \| cerebral infarctions \| 3 C0042384 \| vasculitis \| 2 C0007688 \| central retinal artery occlusion \| 2 C0151295 \| mononeuritis multiplex \| 2 C0035302 \| retinal artery occlusion \| 2 C0010073 \| coronary vasospasm \| 2 C0004096 \| asthma \| 2 C0017658 \| glomerulonephritis \| 2 C0010051 \| coronary aneurysm \| 2 C0027051 \| myocardial infarct \| 2 C0027051 \| myocardial infarction \| 2 C0002871 \| anemia \| 1 C0027121 \| myositis \| 1 C0007785 \| cerebral infarcts \| 1 C0010051 \| coronary aneurysms \| 1 C0015300 \| exophthalmos \| 1 C0017160 \| gastroenteritis \| 1 C0020598 \| hypoglycaemia \| 1 C0021845 \| intestinal perforation \| 1 C0042384 \| angiitis \| 1 C0017661 \| iga glomerulonephritis \| 1 C0553980 \| endomyocardial fibrosis \| 1 C0018801 \| cardiac failure \| 1 C1565662 \| acute renal insufficiency \| 1 C0017668 \| focal segmental glomerulosclerosis \| 1 C0017665 \| membranous nephropathy \| 1 C0178664 \| glomerulosclerosis \| 1 C0751711 \| anterior ischemic optic neuropathy \| 1 C0878544 \| cardiomyopathy \| 1 C0155223 \| dacryoadenitis \| 1 C1527407 \| eosinophilic pneumonia \| 1 C0034065 \| pulmonary embolism \| 1 C1565489 \| renal insufficiency \| 1 C0022658 \| nephropathy \| 1 C0007193 \| dilated cardiomyopathy \| 1 C0017536 \| giardiasis \| 1 C0018202 \| granulomatous angiitis \| 1 C0010073 \| coronary vasospasms \| 1 C0004096 \| bronchial asthma \| 1 C0002878 \| hemolytic anemia \| 1 C0029132 \| optic neuropathy \| 1 C0403416 \| crescentic glomerulonephritis \| 1 C0032285 \| pneumonia \| 1 C0014118 \| endocarditis \| 1 C0002880 \| autoimmune hemolytic anemia \| 1 C0002726 \| amyloidosis \| 1 C0027726 \| nephrotic syndrome \| 1 C0155880 \| intrinsic asthma \| 1 C0456909 \| vision loss \| 1 C0007177 \| cardiac tamponade \| 1 C0026896 \| myasthenia gravis \| 1 C1262481 \| eosinophilic gastroenteritis \| 1 C0155686 \| acute myocarditis \| 1
Curated Gene	(Waiting for update.)
Inferring Gene	Entrez_id \| Symbol \| Resource(Total Genes:5) 3105 \| HLA-A \| infer 3106 \| HLA-B \| infer 3123 \| HLA-DRB1 \| infer 3125 \| HLA-DRB3 \| infer 3126 \| HLA-DRB4 \| infer
Text Mined Gene	Entrez_id \| Symbol \| Score \| Resource(Total Genes:82) 10344 \| CCL26 \| DISEASES 1511 \| CTSG \| DISEASES 6367 \| CCL22 \| DISEASES 6361 \| CCL17 \| DISEASES 333 \| APLP1 \| DISEASES 973 \| CD79A \| DISEASES 4353 \| MPO \| DISEASES 8288 \| EPX \| DISEASES 969 \| CD69 \| DISEASES 3567 \| IL5 \| DISEASES 5657 \| PRTN3 \| DISEASES 2693 \| GHSR \| DISEASES 29108 \| PYCARD \| DISEASES 1401 \| CRP \| DISEASES 5156 \| PDGFRA \| DISEASES 9360 \| PPIG \| DISEASES 23406 \| COTL1 \| DISEASES 671 \| BPI \| DISEASES 3383 \| ICAM1 \| DISEASES 950 \| SCARB2 \| DISEASES 60314 \| C12orf10 \| DISEASES 55023 \| PHIP \| DISEASES 3439 \| IFNA1 \| DISEASES 6749 \| SSRP1 \| DISEASES 2206 \| MS4A2 \| DISEASES 10666 \| CD226 \| DISEASES 9510 \| ADAMTS1 \| DISEASES 55540 \| IL17RB \| DISEASES 5130 \| PCYT1A \| DISEASES 2215 \| FCGR3B \| DISEASES 6778 \| STAT6 \| DISEASES 6037 \| RNASE3 \| DISEASES 3689 \| ITGB2 \| DISEASES 6036 \| RNASE2 \| DISEASES 1493 \| CTLA4 \| DISEASES 375611 \| SLC26A5 \| DISEASES 3596 \| IL13 \| DISEASES 54205 \| CYCS \| DISEASES 2147 \| F2 \| DISEASES 6670 \| SP3 \| DISEASES 10294 \| DNAJA2 \| DISEASES 23786 \| BCL2L13 \| DISEASES 91662 \| NLRP12 \| DISEASES 27181 \| SIGLEC8 \| DISEASES 6605 \| SMARCE1 \| DISEASES 2318 \| FLNC \| DISEASES 8738 \| CRADD \| DISEASES 6401 \| SELE \| DISEASES 11251 \| PTGDR2 \| DISEASES 81608 \| FIP1L1 \| DISEASES 445329 \| SULT1A4 \| DISEASES 3146 \| HMGB1 \| DISEASES 6818 \| SULT1A3 \| DISEASES 3605 \| IL17A \| DISEASES 355 \| FAS \| DISEASES 5265 \| SERPINA1 \| DISEASES 5646 \| PRSS3 \| DISEASES 58 \| ACTA1 \| DISEASES 7042 \| TGFB2 \| DISEASES 9641 \| IKBKE \| DISEASES 149428 \| BNIPL \| DISEASES 959 \| CD40LG \| DISEASES 10800 \| CYSLTR1 \| DISEASES 2268 \| FGR \| DISEASES 6015 \| RING1 \| DISEASES 6257 \| RXRB \| DISEASES 3339 \| HSPG2 \| DISEASES 50943 \| FOXP3 \| DISEASES 7133 \| TNFRSF1B \| DISEASES 780 \| DDR1 \| DISEASES 7056 \| THBD \| DISEASES 2625 \| GATA3 \| DISEASES 1992 \| SERPINB1 \| DISEASES 5660 \| PSAP \| DISEASES 10134 \| BCAP31 \| DISEASES 7124 \| TNF \| DISEASES 3115 \| HLA-DPB1 \| DISEASES 3920 \| LAMP2 \| DISEASES 3586 \| IL10 \| DISEASES 51428 \| DDX41 \| DISEASES 727897 \| MUC5B \| DISEASES 79104 \| MEG8 \| DISEASES
Locus	(Waiting for update.)

Disease ID	1128
Disease	churg-strauss syndrome
Integrated Phenotype	(Waiting for update.)
Text Mined Phenotype	HPO \| Name \| Sentences' Count(Total Phenotypes:50) HP:0002955 \| Granulomatosis \| 25 HP:0012819 \| Myocarditis \| 4 HP:0002633 \| Vasculitis \| 3 HP:0001271 \| Polyneuropathy \| 3 HP:0002138 \| Subarachnoid hemorrhage \| 2 HP:0000099 \| Glomerular nephritis \| 2 HP:0001658 \| Myocardial infarction \| 2 HP:0001342 \| Intracerebral hemorrhage \| 2 HP:0002099 \| Asthma \| 2 HP:0002617 \| Aneurysmal dilatation \| 2 HP:0000572 \| Visual loss \| 1 HP:0002113 \| Pulmonary infiltrates \| 1 HP:0000520 \| Anterior bulging of the globe of eye \| 1 HP:0001878 \| Haemolytic anaemia \| 1 HP:0002105 \| Hemoptysis \| 1 HP:0100582 \| Nasal polyps \| 1 HP:0002090 \| Pneumonia \| 1 HP:0030149 \| Cardiovascular shock \| 1 HP:0000100 \| Nephrosis \| 1 HP:0001685 \| Myocardial fibrosis \| 1 HP:0001890 \| Autoimmune hemolytic anemia \| 1 HP:0001410 \| Decreased liver function \| 1 HP:0003473 \| Fatigable weakness \| 1 HP:0011034 \| Amyloid disease \| 1 HP:0000097 \| focal glomerulosclerosis \| 1 HP:0001635 \| Congestive heart failure \| 1 HP:0008653 \| Crescentic glomerulonephritis \| 1 HP:0001903 \| Anemia \| 1 HP:0002027 \| Abdominal pain \| 1 HP:0001291 \| Cranial nerve disease \| 1 HP:0000096 \| Glomerulosclerosis \| 1 HP:0001880 \| Eosinophilia \| 1 HP:0100614 \| Muscle inflammation \| 1 HP:0000365 \| Hearing impairment \| 1 HP:0002204 \| Pulmonary embolism \| 1 HP:0000112 \| Nephropathy \| 1 HP:0012531 \| Pain \| 1 HP:0001943 \| Hypoglycemia \| 1 HP:0010604 \| Cyst of the eyelid \| 1 HP:0002597 \| Abnormality of blood vessels \| 1 HP:0000083 \| Renal insufficiency \| 1 HP:0001919 \| Acute renal failure \| 1 HP:0001138 \| Damaged optic nerve \| 1 HP:0001917 \| Renal amyloidosis \| 1 HP:0006685 \| Endocardial fibrosis \| 1 HP:0001644 \| Congestive cardiomyopathy \| 1 HP:0001638 \| Cardiomyopathy \| 1 HP:0003613 \| Antiphospholipid antibodies \| 1 HP:0100584 \| Endocarditis \| 1 HP:0012578 \| Membranous glomerulonephritis \| 1

Disease ID	1128
Disease	churg-strauss syndrome
Manually Symptom	(Waiting for update.)
Text Mined Symptom	UMLS \| Name \| Sentences' Count(Total Symptoms:20) C0027059 \| myocarditis \| 4 C0151788 \| eosinophilic myocarditis \| 4 C0235880 \| mononeuritis \| 3 C0442874 \| neuropathy \| 3 C0019080 \| hemorrhage \| 3 C0007785 \| cerebral infarctions \| 3 C0152025 \| polyneuropathy \| 3 C0343192 \| microscopic polyangiitis \| 2 C0042384 \| vasculitis \| 2 C0553980 \| endomyocardial fibrosis \| 1 C0029132 \| optic neuropathy \| 1 C0334108 \| polyposis \| 1 C0002940 \| aneurysms \| 1 C0751711 \| anterior ischemic optic neuropathy \| 1 C0014457 \| eosinophilia \| 1 C0007688 \| central retinal artery occlusion \| 1 C2350476 \| orbital myositis \| 1 C0027726 \| nephrotic syndrome \| 1 C0042384 \| angiitis \| 1 C0878544 \| cardiomyopathy \| 1

Manually Genotype(Total Text Mining Genotypes:0)
(Waiting for update.)

All Snps(Total Genotypes:0)
(Waiting for update.)

GWASdb Annotation(Total Genotypes:0)
(Waiting for update.)

GWASdb Snp Trait(Total Genotypes:0)
(Waiting for update.)

Mapped by lexical matching(Total Items:0)
(Waiting for update.)

Mapped by homologous gene(Total Items:0)
(Waiting for update.)

Chemical(Total Drugs:8)
CUI	ChemicalName	ChemicalID	CasRN	DiseaseName	DiseaseID	DirectEvidence	PubMedIDs
C0008728	acetaminophen	D000082	103-90-2	churg-strauss syndrome	MESH:D015267	marker/mechanism	15942102
C0008728	azithromycin	D017963	83905-01-5	churg-strauss syndrome	MESH:D015267	marker/mechanism	9555706
C0008728	carbamazepine	D002220	298-46-4	churg-strauss syndrome	MESH:D015267	marker/mechanism	2918954
C0008728	carbimazole	D002231	22232-54-8	churg-strauss syndrome	MESH:D015267	marker/mechanism	16018796
C0008728	cyclophosphamide	D003520	50-18-0	churg-strauss syndrome	MESH:D015267	therapeutic	14756469
C0008728	montelukast	C093875	158966-92-8	churg-strauss syndrome	MESH:D015267	marker/mechanism	12958007
C0008728	phenytoin	D010672	57-41-0	churg-strauss syndrome	MESH:D015267	marker/mechanism	3753844
C0008728	zafirlukast	C062735	107753-78-6	churg-strauss syndrome	MESH:D015267	marker/mechanism	10073523

FDA approved drug and dosage information(Total Drugs:4)
DiseaseID	Drug_name	active_ingredients	strength	Dosage Form/Route	Marketing Status	TE code	RLD	RS
MESH:D015267	ofirmev	acetaminophen	1GM/100ML (10MG/ML)	SOLUTION;IV (INFUSION)	Prescription	AP	Yes	Yes
MESH:D015267	ofirmev	acetaminophen	1GM/100ML (10MG/ML)	SOLUTION;IV (INFUSION)	Prescription	AP	Yes	Yes
MESH:D015267	acetaminophen	acetaminophen	650MG	SUPPOSITORY;RECTAL	Over-the-counter	None	Yes	Yes
MESH:D015267	acetaminophen	acetaminophen	650MG	SUPPOSITORY;RECTAL	Over-the-counter	None	Yes	Yes

FDA labeling changes(Total Drugs:4)
DiseaseID	Pediatric_Labeling_Date	Trade_Name	Generic_Name_or_Proper_Name	Indications Studied	Label Changes Summary	Product Labeling	BPCA(B)	PREA(P)	BPCA(B) and PREA(P)	Pediatric Rule (R)	Sponsor	Pediatric Exclusivity Granted Date	NNPS
MESH:D015267	2/11/2010	ofirmev	acetaminophen	Management of mild-to-moderate pain, for the management of moderate-to-severe pain with adjunctive opioid analgesics, and for the reduction of fever	The safety and effectiveness of Ofirmev for the treatment of acute pain and fever in pediatric patients ages 2 years and older is supported by evidence from adequate and well-controlled studies of Ofirmev in adults. Additional safety and PK data was collected in 355 from premature neonates to adolescents. The effectiveness of Ofirmev for the treatment of acute pain and fever has not been studied in pediatric patients < 2 years of age.The PK exposure of Ofirmev observed in children and adolescents is similar to adults, but higher in neonates and infants. Dosing simulations from PK data in infants and neonates suggest that dose reductions of 33% in infants 1 month to < 2 years of age, and 50% in neonates up to 28 days, with a minimum dosing interval of 6 hours, will produce a PK exposure similar to that observed in children age 2 years and olderMost common adverse reactions in pediatric patients were nausea, vomiting, constipation, pruritus, agitation, and atelectasis.Information on dosing, clinical studies, adverse reactions and PK parametersNew dosage form and route of administration	Labeling	-	P	-	-	Cadence	-	FALSE'
MESH:D015267	01/27/2017	ofirmev	acetaminophen	Treatmeny of pain and fever in pediatric patients birth to 2 years	Treatment of pain Efficacy was not demonstrated in pediatric patients younger than 2 years in a double-blind, placebo-controlled study of 198 pediatric patients younger than 2 years. Pediatric patients less than 2 years of age, including neonates from 28 to 40 weeks gestational age at birth, were randomized to receive opioid plus acetaminophen or opioid plus placebo. No difference in analgesic effect of intravenous acetaminophen, measured by assessment of reduced need for additional opioid treatment for pain control, was observed. Treatment of fever The safety and effectiveness for the treatment of fever in pediatric patients, including premature neonates born at 32 weeks or greater gestation is supported by adequate and well-controlled studies of Ofirmev in adults, clinical studies in 244 pediatric patients 2 years and older, and safety and pharmacokinetic data from 239 patients younger than 2 years including neonates 32 weeks or greater gestational age. Information on dosing, clinical trials. Postmarketing study.	Labeling	-	-	B,P	-	Mallinckrodt	11/7/2016	FALSE
MESH:D015267	2/11/2010	ofirmev	acetaminophen	Management of mild-to-moderate pain, for the management of moderate-to-severe pain with adjunctive opioid analgesics, and for the reduction of fever	The safety and effectiveness of Ofirmev for the treatment of acute pain and fever in pediatric patients ages 2 years and older is supported by evidence from adequate and well-controlled studies of Ofirmev in adults. Additional safety and PK data was collected in 355 from premature neonates to adolescents. The effectiveness of Ofirmev for the treatment of acute pain and fever has not been studied in pediatric patients < 2 years of age.The PK exposure of Ofirmev observed in children and adolescents is similar to adults, but higher in neonates and infants. Dosing simulations from PK data in infants and neonates suggest that dose reductions of 33% in infants 1 month to < 2 years of age, and 50% in neonates up to 28 days, with a minimum dosing interval of 6 hours, will produce a PK exposure similar to that observed in children age 2 years and olderMost common adverse reactions in pediatric patients were nausea, vomiting, constipation, pruritus, agitation, and atelectasis.Information on dosing, clinical studies, adverse reactions and PK parametersNew dosage form and route of administration	Labeling	-	P	-	-	Cadence	-	FALSE'
MESH:D015267	01/27/2017	ofirmev	acetaminophen	Treatmeny of pain and fever in pediatric patients birth to 2 years	Treatment of pain Efficacy was not demonstrated in pediatric patients younger than 2 years in a double-blind, placebo-controlled study of 198 pediatric patients younger than 2 years. Pediatric patients less than 2 years of age, including neonates from 28 to 40 weeks gestational age at birth, were randomized to receive opioid plus acetaminophen or opioid plus placebo. No difference in analgesic effect of intravenous acetaminophen, measured by assessment of reduced need for additional opioid treatment for pain control, was observed. Treatment of fever The safety and effectiveness for the treatment of fever in pediatric patients, including premature neonates born at 32 weeks or greater gestation is supported by adequate and well-controlled studies of Ofirmev in adults, clinical studies in 244 pediatric patients 2 years and older, and safety and pharmacokinetic data from 239 patients younger than 2 years including neonates 32 weeks or greater gestational age. Information on dosing, clinical trials. Postmarketing study.	Labeling	-	-	B,P	-	Mallinckrodt	11/7/2016	FALSE

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