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Pachyonychia Congenita Gene_reviews

International Pachyonychia Congenita Research Registry (IPCRR) Data Summary (as of 10 May 2017) View in own window Gene in Which Pathogenic Variants Were Confirmed KRT6A KRT6B KRT6C KRT16 KRT17 TOTAL Number evaluated for finding 1 304 71 22 247 130 774 Toenails thickened 10 toenails 286 (94%) 26 (37%) 0 (00%) 99 (40%) 100 (77%) 511 (66%) 7-9 toenails 9 (03%) 14 (20%) 0 (00%) 52 (21%) 11 (08%) 86 (11%) 4-6 toenails 2 (01%) 21 (30%) 3 (14%) 63 (26%) 7 (05%) 96 (12%) 1-3 toenails 4 (01%) 9 (13%) 10 (45%) 44 (18%) 8 (06%) 75 (10%) Total w/toenails thickened 301 (99%) 70 (99%) 13 (59%) 238 (96%) 126 (97%) 748 (97%) Age at onset Birth - <1 yr 264 (88%) 10 (14%) 1 (08%) 45 (19%) 92 (73%) 412 (54%) 1-4 yrs 33 (11%) 19 (27%) 6 (46%) 78 (33%) 24 (19%) 160 (21%) 5-14 yrs 4 (01%) 34 (49%) 4 (31%) 74 (31%) 10 (08%) 126 (17%) ≥15 yrs 0 (00%) 7 (10%) 2 (15%) 43 (18%) 1 (01%) 53 (07%) Fingernails thickened 10 fingernails 271 (89%) 4 (06%) 0 (00%) 73 (30%) 62 (48%) 410 (53%) 7-9 fingernails 10 (03%) 4 (06%) 0 (00%) 11 (04%) 13 (10%) 38 (05%) 4-6 fingernails 14 (05%) 17 (24%) 0 (00%) 30 (12%) 28 (22%) 89 (11%) 1-3 fingernails 6 (02%) 7 (10%) 0 (00%) 28 (11%) 9 (07%) 50 (06%) Total w/fingernails thickened 301 (99%) 32 (45%) 0 (00%) 142 (57%) 112 (86%) 587 (76%) Age at onset Birth - <1 yr 267 (89%) 4 (13%) 0 (00%) 33 (23%) 85 (76%) 389 (66%) 1-4 yrs 30 (10%) 8 (25%) 0 (00%) 42 (30%) 19 (17%) 99 (17%) 5-14 yrs 3 (01%) 11 (34%) 0 (00%) 34 (24%) 6 (05%) 54 (09%) ≥15 yrs 1 (00%) 10 (31%) 0 (00%) 34 (24%) 3 (03%) 48 (08%) Plantar keratoderma Always (never completely goes away) 254 (84%) 67 (94%) 19 (86%) 240 (97%) 86 (66%) 666 (86%) Sometimes (feet clear up completely at times) 7 (02%) 1 (01%) 0 (00%) 1 (00%) 14 (11%) 23 (03%) Seldom (feet usually clear of symptoms) 5 (02%) 0 (00%) 0 (00%) 0 (00%) 4 (03%) 9 (01%) Total w/plantar keratoderma 266 (88%) 68 (96%) 19 (86%) 241 (98%) 104 (80%) 698 (90%) Age at onset Birth - <1 yr 39 (15%) 2 (03%) 1 (05%) 23 (10%) 12 (12%) 77 (11%) 1-4 yrs 152 (57%) 23 (34%) 9 (47%) 130 (54%) 35 (34%) 349 (50%) 5-14 yrs 70 (26%) 42 (62%) 9 (47%) 82 (34%) 43 (41%) 246 (35%) ≥15 yrs 5 (02%) 1 (01%) 0 (00%) 8 (03%) 15 (14%) 29 (04%) Plantar pain w/plantar keratoderma 2 Often require medication for pain 65 (24%) 12 (18%) 5 (26%) 74 (31%) 19 (18%) 175 (25%) Very painful, but do not use medication 114 (43%) 32 (47%) 11 (58%) 111 (46%) 34 (33%) 302 (43%) Somewhat painful 77 (29%) 24 (35%) 3 (16%) 50 (21%) 36 (35%) 190 (27%) Total w/plantar keratoderma/pain 256 (96%) 68 (100%) 19 (100%) 235 (98%) 89 (86%) 667 (96%) Palmar keratoderma Always (never completely goes away) 86 (28%) 11 (15%) 2 (09%) 148 (60%) 21 (16%) 268 (35%) Sometimes (hands clear up completely at times) 32 (11%) 7 (10%) 1 (05%) 15 (06%) 22 (17%) 77 (10%) Seldom (hands usually clear of symptoms) 49 (16%) 13 (18%) 3 (14%) 22 (09%) 27 (21%) 114 (15%) Total w/palmar keratoderma 167 (55%) 31 (44%) 6 (27%) 185 (75%) 70 (54%) 459 (59%) Additional findings Oral leukokeratosis 269 (88%) 18 (25%) 4 (18%) 88 (36%) 34 (26%) 413 (53%) Cysts 188 (62%) 49 (69%) 4 (18%) 64 (26%) 121 (93%) 426 (55%) Follicular hyperkeratosis 162 (53%) 30 (42%) 0 (00%) 30 (12%) 86 (66%) 308 (40%) Natal or prenatal teeth 12 (04%) 0 (00%) 0 (00%) 0 (00%) 99 (76%) 111 (14%) 1.

KRT17, KRT16, KRT6A, KRT6B, KRT10, KRT6C, KRT80, SLURP1, PNOC, NFE2L2, AQP5, FLG, KRT1, KLKB1, GJB2, GABPA, MTOR, KRT9
- Pachyonychia Congenita 4 Omim
  
  A number sign (#) is used with this entry because pachyonychia congenita-4 (PC4) is caused by heterozygous mutation in the KRT6B gene (148042) on chromosome 12q13. Description Pachyonychia congenita (PC) is an autosomal dominant genodermatosis with the main clinical features of hypertrophic nail dystrophy, painful and highly debilitating plantar keratoderma, oral leukokeratosis, and a variety of epidermal cysts. Although the condition had previously been subdivided clinically into Jadassohn-Lewandowsky PC type 1 and Jackson-Lawler PC type 2, patients with PC were later found to have a mixed constellation of both types, leading to a classification of PC based on genotype (summary by Sybert, 2010; Eliason et al., 2012; McLean et al., 2011). For a discussion of genetic heterogeneity of pachyonychia congenita, see 167200. Historical Classification of Pachyonychia Congenita Gorlin et al. (1976) suggested that 2 distinct syndromes are subsumed under the designation pachyonychia congenita.
- Pachyonychia Congenita Orphanet
  
  Pachyonychia congenita (PC) is a rare genodermatosis predominantly featuring painful palmoplantar keratoderma, thickened nails, cysts and whitish oral mucosa. Epidemiology The prevalence is not known but approximately 1000 patients have been registered to date worldwide. Clinical description PC presents clinically as a spectrum of conditions. PC onset is variable with most cases manifesting soon after birth, others becoming clinically apparent only in late childhood and rarely in adulthood. The first signs of the disease usually are thickened nails or neonatal teeth.
- Pachyonychia Congenita Gard
  
  Pachyonychia congenita (PC) is a rare inherited condition that primarily affects the nails and skin. The fingernails and toenails may be thickened and abnormally shaped . Affected people can also develop painful calluses and blisters on the soles of their feet and less frequently on the palms of their hands ( palmoplantar keratoderma ). Additional features include white patches on the tongue and inside of the mouth (leukokeratosis); bumps around the elbows, knees, and waistline (follicular hyperkeratosis); and cysts of various types including steatocystoma. Features may vary among affected people depending on their specific mutation.
- Pachyonychia Congenita, Autosomal Recessive Omim
  
  For a phenotypic description and a discussion of genetic heterogeneity of pachyonychia congenita, see 167200. Inheritance Chong-Hai and Rajagopalan (1977) suggested autosomal recessive inheritance of pachyonychia congenita in a 4-year-old Malaysian girl with first-cousin parents, although they recognized new dominant mutation as a possibility. See also Sivasundram et al. (1985). INHERITANCE - Autosomal recessive HEAD & NECK Mouth - No oral leukoplakia SKIN, NAILS, & HAIR Skin - Horny papules (face, leg, buttocks) - No palmoplantar hyperkeratosis - No hyperhidrosis Nails - Episodic inflammatory swelling of nail bed - Recurrent shedding of nails - Hard,thickened nails (pachyonychia) - Subungual hyperkeratosis MISCELLANEOUS - See also pachyonychia congenita, type 3 (PC1, 167200 ) ▲ Close
- Pachyonychia Congenita 3 Omim
  
  A number sign (#) is used with this entry because pachyonychia congenita-3 (PC3) is caused by heterozygous mutation in the keratin-6a gene (KRT6A; 148041) on chromosome 12q13. Description Pachyonychia congenita (PC) is an autosomal dominant genodermatosis with the main clinical features of hypertrophic nail dystrophy, painful and highly debilitating plantar keratoderma, oral leukokeratosis, and a variety of epidermal cysts. Although the condition had previously been subdivided clinically into Jadassohn-Lewandowsky PC type 1 and Jackson-Lawler PC type 2, patients with PC were later found to have a mixed constellation of both types, leading to a classification of PC based on genotype (summary by Sybert, 2010; Eliason et al., 2012; McLean et al., 2011). For a discussion of genetic heterogeneity of pachyonychia congenita, see 167200. Historical Classification of Pachyonychia Congenita Gorlin et al. (1976) suggested that 2 distinct syndromes are subsumed under the designation pachyonychia congenita.
- Pachyonychia Congenita 2 Omim
  
  A number sign (#) is used with this entry because of evidence that pachyonychia congenita-2 (PC2) is caused by heterozygous mutation in the KRT17 gene (148069) on chromosome 17q21. Description Pachyonychia congenita (PC) is an autosomal dominant genodermatosis with the main clinical features of hypertrophic nail dystrophy, painful and highly debilitating plantar keratoderma, oral leukokeratosis, and a variety of epidermal cysts. Although the condition had previously been subdivided clinically into Jadassohn-Lewandowsky PC type 1 and Jackson-Lawler PC type 2, patients with PC were later found to have a mixed constellation of both types, leading to a classification of PC based on genotype (summary by Sybert, 2010; Eliason et al., 2012; McLean et al., 2011). For a discussion of genetic heterogeneity of pachyonychia congenita, see 167200. Historical Classification of Pachyonychia Congenita Gorlin et al. (1976) suggested that 2 distinct syndromes are subsumed under the designation pachyonychia congenita.
- Pachyonychia Congenita 1 Omim
  
  A number sign (#) is used with this entry because pachyonychia congenita-1 (PC1) is caused by heterozygous mutation in the keratin-16 gene (KRT16; 148067) on chromosome 17q21. Description Pachyonychia congenita (PC) is an autosomal dominant genodermatosis with the main clinical features of hypertrophic nail dystrophy, painful and highly debilitating plantar keratoderma, oral leukokeratosis, and a variety of epidermal cysts. Although the condition had previously been subdivided clinically into Jadassohn-Lewandowsky PC type 1 and Jackson-Lawler PC type 2, patients with PC were later found to have a mixed constellation of both types, leading to a classification of PC based on genotype (summary by Sybert, 2010; Eliason et al., 2012; McLean et al., 2011). Historical Classification of Pachyonychia Congenita Gorlin et al. (1976) suggested that 2 distinct syndromes are subsumed under the designation pachyonychia congenita. PC type 1, the Jadassohn-Lewandowsky type, shows oral leukokeratosis.
Hydroa Vacciniforme Wikipedia

A study by Iwatsuki et al. detected Epstein-Barr virus (EBV) positive T-cells in the perivascular infiltration on biopsy in 28/29 patients tested. Antibody titers to EBV were measured in 14 of these patients and only five had abnormal antibody patterns consistent with chronic active EBV infection. [6] Treatment [ edit ] Antiviral treatment has been tried with some success in a small number of patients. [7] See also [ edit ] List of cutaneous conditions Epstein-Barr virus References [ edit ] ^ Bazin, E (1862). ... Feb, 42(2 Pt 1) (2): 208–13. doi : 10.1016/s0190-9622(00)90127-0 . PMID 10642674 . ^ James, William D.; Berger, Timothy G.; et al. (2006). Andrews' Diseases of the Skin: clinical Dermatology . Saunders Elsevier. ISBN 0-7216-2921-0 . ^ Rezk SA, Zhao X, Weiss LM (September 2018).

CD4, CCR4, GATA2, PLK2
- Hydroa Vacciniforme Orphanet
  
  A rare photodermatosis characterized by the development of pruritic or painful vesicles in a photodistributed pattern in response to sunlight exposure. The lesions heal with permanent varioliform scarring. Ocular involvement, deformities of ears and nose, or contractures of the fingers may occasionally be observed. Systemic signs and symptoms are absent. The condition typically occurs in childhood and regresses spontaneously in adolescence or young adulthood.
Primary And Secondary Brain Injury Wikipedia

Hagerstown, MD: Lippincott Williams & Wilkins. p. 1150. ISBN 0-7817-2655-7 . Retrieved 2008-06-16 . ^ a b c d e f Scalea TM (2005). ... Boca Raton: CRC. pp. 26–32. ISBN 978-0-8493-8138-6 . Retrieved 2008-07-06 . ^ a b Porth, Carol (2007). ... Hagerstown, MD: Lippincott Williams & Wilkins. p. 838. ISBN 978-0-7817-7087-3 . Retrieved 2008-07-03 . ^ Pitkänen A, McIntosh TK (2006). ... Neurotrauma: New Insights Into Pathology and Treatment . Elsevier. pp. 13–19. ISBN 978-0-444-53017-2 . Retrieved 2008-06-10 . ^ a b Granacher RP (2007). ... Neuroscience . 101 (2): 289–95. doi : 10.1016/S0306-4522(00)00380-8 . PMID 11074152 . S2CID 20457228 . ^ Sauaia A, Moore FA, Moore EE, et al.
Botellón Wikipedia

Characteristics [ edit ] Botellón usually begins around 11:00 p.m. and ends around 3:00 a.m. when many people move to a bar or club. ... Since botellón is usually a nighttime activity, Spain passed a law that prohibits stores to sell alcohol to the public after 10:00 p.m, hoping to persuade people to attend clubs or bars where alcohol must remain on site. [ citation needed ] However, the measure is a controversial one because people can still buy alcohol before the selling limit hour and consume it in public. ... Alicante: El Mundo. 9 March 2010. ^ Reyes Rincón (28 November 2006). "Nace el 'botellódromo':El Ayuntamiento de Granada construye un espacio a las afueras de la ciudad para que 20.000 jóvenes puedan beber sin molestia" . ... CS1 maint: archived copy as title ( link ) ^ "Media España se cita en la Red para celebrar un macrobotellón el 17 de marzo" . 2006-03-07. ^ http://www.20minutos.es/noticia/97295/0/macrobotellones/ciudades/espana/ | Literally translated from Spanish ^ "El Ayuntamiento "no consentirá" el macrobotellón que se prepara en Moncloa" . 2006-03-07.
Epithelioma Wikipedia

. ^ "Deaths in the district of Inveresk and Musselburgh in the County of Edinburgh" . Statutory Deaths 689/00 0032 . ScotlandsPeople . Retrieved 11 April 2015 . External links [ edit ] Classification D ICD-O : 8011/0, 8011/3 Wikimedia Commons has media related to Epithelioma .

AS3MT, LATS1, HPGD, SCD, ERBB2, MUC1, EGFR, TP53, CTNNB1, CD274, VEGFA, CDKN2A, FHIT, CD44, EPCAM, BCL2, NCOA3, ANIB1, HEATR6, VIM, PTK6, KIT, FAP, IGF1, CD82, NTRK1, PIK3CG, EGF, KRAS, PIK3CD, GLI1, RASSF1, PIK3CB, MMP2, PIK3CA, SRA1, GTF2I, H3P10, MIR21, MIR200C, NPC1, MTA1, LINC01194, FSHR, FSCN1, CLU, BRAF, HGF, ABCB1, FOXL2, PDLIM7, PCNA, SMUG1, NOTCH1, FGF2, BAX, TBC1D9, CXCL8, MYB, ITGAE, JAG2, MICA, TNF, KRT19, LGALS1, TRBV20OR9-2, MMP14, MMP9, PPARG, FST, FASN, EZH2, PTGS2, VHL, ODAM, EPHB4, FOXN1, ESR1, MUC16, CRP, PROM1, CLDN3, RUNX3, NUTM1, SGK1, WT1, TSC1, VTN, NR0B2, BCL2L10, CXCR4, SLC7A5, TMPRSS2, BCL2L11, TIMP2, TRIM13, PAX8, ZNF154, TIMP1, TSC2, UVRAG, NR1I3, FEZ1, UMPS, NEURL1, TYMS, TTR, CFLAR, RIPK1, CDK2AP2, TP63, KLF4, COX5A, EI24, TTN, CXCL14, KLK4, TTF1, LMO4, HSPB3, XPO1, CASP14, SEMA3C, DIAPH3, TXLNA, IMMP1L, ARX, IRX2, MLIP, MARVELD1, HM13, FBXW7, SLC44A4, PHC3, LIN28A, C19orf33, LGR6, OVOL2, MUC20, PGP, LYPD5, MIR141, MIR143, MIR145, MIR148A, MIR214, MIR485, CXADRP1, TEC, KLRC4-KLRK1, ERVK-20, ERVK-18, AK6, ERVK-32, H3P8, SLC12A9, TRIM62, UBD, CYFIP1, CLIC4, FBXO7, TRIM29, TGFB2, SATB2, FBXW11, KLRK1, ERCC6L, RPP14, CKAP4, SUB1, FASTK, IGF2BP1, PDPN, NOC2L, NOX1, IL17C, LAMTOR2, HIPK2, ERVW-1, FOXP3, APH1A, EGFL7, LEF1, HSD17B7, SF3B6, ACSL5, WWOX, RTEL1, WNT4, KRT20, THM, ACTB, TFPI, FGF7, CTSV, CXADR, CYP19A1, DAXX, DPYD, DSG2, EIF2S1, ELF3, ELF4, EN1, EWSR1, F2R, F3, FBLN1, FGFR2, CSF1, FN1, FOLH1, FRA16D, GPC3, HAS1, HHEX, HIF1A, HIP1, HLA-G, HMGB1, HMGA1, HNF4A, HOXA7, HRAS, CSF1R, CPOX, TFE3, CA9, AKT1, ALCAM, ALOX5, ANXA2, BIRC2, BIRC3, FAS, AR, ARR3, BGLAP, CEACAM1, BRCA1, BRCA2, TSPO, CASP8, COX8A, CASR, CAT, CAV1, RUNX1, MS4A1, CD40, CD68, CD70, CD74, CDC42, CDH1, CDKN1A, CDKN2B, CEACAM5, ERAS, HSF1, HSPB1, CXCL11, MAP2K1, PTCH1, PTEN, PTK2, PTPN6, PTPRJ, PXN, AFP, RAP2B, RARB, RPE65, S100A1, S100A9, S100B, SDC1, HSPB2, SFPQ, SFRP5, SLC22A1, SNAI2, SNAI1, SOX2, SPG7, SPP1, SRC, ST14, ADAM17, TBX5, ZEB1, TERT, MAPK7, PRKAR1A, POU2F1, PLK1, IFNA1, IFNA13, IGF1R, IGFBP7, IL2, IL4, IL6, IPP, KRT17, LAG3, LEP, MDK, MEIS1, MET, KITLG, MGMT, MST1R, MUC4, MYC, NEU1, NFIB, NOTCH3, ROR1, ODC1, OVOL1, PAX1, PDGFA, PDGFRB, PLAU, RAG1
Mouse Model Of Colorectal And Intestinal Cancer Wikipedia

A diet-related mouse model of colon cancer was devised. [28] [29] In this model, wild type mice are fed a standard diet plus DOC to give a level of DOC in mouse colon comparable to that in the colons of humans on a high fat diet. [28] After 8–10 months, 45% to 56% of the mice developed colonic adenocarcinomas , and no mice had cancers of the small intestine. ... PMID 26295972 . ^ Oh, BY; Hong, HK; Lee, WY; Cho, YB (28 February 2017). "Animal models of colorectal cancer with liver metastasis". ... Cell . 66 (3): 589–600. doi : 10.1016/0092-8674(81)90021-0 . PMID 1651174 . ^ Moser AR, Pitot HC, Dove WF (1990). ... Cell . 92 (5): 645–56. doi : 10.1016/S0092-8674(00)81132-0 . PMID 9506519 . ^ Kolodner R (1996). ... Cell . 91 (4): 467–77. doi : 10.1016/S0092-8674(00)80433-X . PMID 9390556 . ^ Reitmair AH, Redston M, Cai JC, et al. (1996).
Fudan Poisoning Case Wikipedia

Police immediately organized a task force to conduct an investigation. About 0:00 on April 12, 2013, after the police determined that Lin was a suspect and summoned him, Lin then confessed that he had put N -nitrosodimethylamine in dorm 421's water dispenser. ... According to defence lawyer Xie Tonxiang, the chief justice agreed to meet the defendant's father, Lin Zunyao, on July 28 2015. Lin Zunyao and the chief justice discussed the case in the courtroom of the Supreme People's Court. ... Archived from the original on 2015-04-21. ^ "上海一周：反思"复旦投毒案"中的舆论角色" . 163.com . 2014-02-24. Archived from the original on 2015-01-25. ^ "最高法复核复旦投毒案被告人死刑判决" .
Gilbert's Syndrome Wikipedia

"Frequent co-occurrence of the TATA box mutation associated with Gilbert's syndrome (UGT1A1*28) with other polymorphisms of the UDP-glucuronosyltransferase-1 locus (UGT1A6*2 and UGT1A7*3) in Caucasians and Egyptians". ... S2CID 43486067 . ^ Schwertner Harvey A; Vítek Libor (May 2008). "Gilbert syndrome, UGT1A1*28 allele, and cardiovascular disease risk: possible protective effects and therapeutic applications of bilirubin" . ... PMID 11849670 . ^ Lin JP; O’Donnell CJ; Schwaiger JP; et al. (2006). "Association between the UGT1A1*28 allele, bilirubin levels, and coronary heart disease in the Framingham Heart Study" . ... Greenwood Publishing Group. pp. 175 . ISBN 978-0-313-33528-0 . ^ "Wire preaches delights of three cliffs". ... "Illness that 'shut down' Tech3 MotoGP rookie Jonas Folger diagnosed" . Autosport .com . Motorsport Network . Retrieved 2017-11-09 .

UGT1A1, UGT1A, UGT1A10, UGT1A8, UGT1A7, UGT1A6, UGT1A4, UGT1A3, UGT1A5, UGT1A9, SLC35A2, G6PD, UGGT1, HFE, CNDP2, CHPT1, ABCG5, DHDDS, NT5C3A, NT5C2, UROD, NAT2, ABO, SLC10A2, ACP3, ABCC2, CYP2D7, CYP2D6, DPYD, GPT, IBSP, IL1B, IL6, NT5E, PPARA, PRKAA1, PRKAA2, PRKAB1, SELP, LOC107987479
- Gilbert Syndrome Mayo_clinic
  
  Overview Gilbert (zheel-BAYR) syndrome is a common, harmless liver condition in which the liver doesn't properly process bilirubin. Bilirubin is produced by the breakdown of red blood cells. The liver The liver is your largest internal organ. About the size of a football, it's located mainly in the upper right portion of your abdomen, beneath the diaphragm and above your stomach. Gilbert syndrome is an inherited genetic condition. You might not know you have Gilbert syndrome until it's discovered by accident, such as when a blood test shows raised bilirubin levels. Gilbert syndrome requires no treatment. Symptoms The most frequent sign of Gilbert syndrome is an occasional yellowish tinge of the skin and the whites of the eyes as a result of slightly higher levels of bilirubin in the blood.
- Gilbert Syndrome Medlineplus
  
  In many populations, the most common genetic change that causes Gilbert syndrome (known as UGT1A1*28) occurs in an area near the UGT1A1 gene called the promoter region, which controls the production of the bilirubin-UGT enzyme. ... When the condition is caused by the UGT1A1*28 change in the promoter region of the UGT1A1 gene, it is inherited in an autosomal recessive pattern , which means both copies of the gene in each cell have the mutation.
- Gilbert Syndrome Omim
  
  A number sign (#) is used with this entry because Gilbert syndrome is caused by homozygous, compound heterozygous, or heterozygous mutation in the UDP-glucuronosyltransferase gene (UGT1A1; 191740) on chromosome 2q37. Description The hereditary hyperbilirubinemias (Wolkoff et al., 1983) include (1) those resulting in predominantly unconjugated hyperbilirubinemia: Gilbert or Arias syndrome, Crigler-Najjar syndrome type I (218800), and Crigler-Najjar syndrome type II (606785); and (2) those resulting in predominantly conjugated hyperbilirubinemia: Dubin-Johnson syndrome (237500), Rotor syndrome (237450), and several forms of intrahepatic cholestasis (147480, 211600, 214950, 243300). Detailed studies show that patients with Gilbert syndrome have reduced activity of bilirubin glucuronosyltransferase (Bosma et al., 1995, Koiwai et al., 1995). Genetic Heterogeneity of Hyperbilirubinemia See also Crigler-Najjar syndrome type I (HBLRCN1; 218800), Crigler-Najjar syndrome type II (HBLRCN2; 606785), and transient familial neonatal hyperbilirubinemia (HBLRTFN; 237900), all caused by mutation in the UGT1A1 gene (191740) on chromosome 2q37; Dubin-Johnson syndrome (DJS, HBLRDJ; 237500), caused by mutation in the ABCC2 gene (601107) on chromosome 10q24; and Rotor syndrome (HBLRR; 237450), caused by digenic mutation in the SLCO1B1 (604843) and SLCOB3 (605495) genes, both on chromosome 12p. Clinical Features The characteristics of Gilbert syndrome are normal liver function tests of the usual type, normal liver histology, delayed clearance of bilirubin from the blood, and mild jaundice that tends to fluctuate in severity, particularly after fasting (Nixon and Monahan, 1967).
Staphylococcal Scalded Skin Syndrome Wikipedia

The Lancet . 156 (4011): 89–95. doi : 10.1016/S0140-6736(00)65681-7 . ^ Weisse, Martin E (31 December 2000). ... The Lancet . 357 (9252): 299–301. doi : 10.1016/S0140-6736(00)03623-0 . PMID 11214144 . S2CID 35896288 . ^ Powell, KR (January 1979). ... The Journal of Pediatrics . 78 (6): 958–67. doi : 10.1016/S0022-3476(71)80425-0 . PMID 4252715 . ^ Morens, David M; Katz, Alan R; Melish, Marian E (31 May 2001). ... The Lancet . 357 (9273): 2059. doi : 10.1016/S0140-6736(00)05151-5 . PMID 11441870 . S2CID 35925579 .

DSG1, EDNRB, EDNRA, EXT1, SPINK5, SETBP1, DSG4
- Staphylococcal Scalded Skin Syndrome Orphanet
  
  A rare staphylococcal toxemia caused by epidermolytic toxins of Staphylococcus aureus and characterized by the appearance of widespread erythematous patches, on which large blisters develop. Upon rupture of these blisters, the skin appears reddish and scalded. The lesions typically begin in the face and rapidly expand to other parts of the body. The disease may be complicated by pneumonia and sepsis. It most commonly affects newborns and infants.
Dukes' Disease Wikipedia

The Lancet . 156 (4011): 89–95. doi : 10.1016/S0140-6736(00)65681-7 . ^ a b c d Weisse, ME (31 December 2000). ... The Lancet . 357 (9252): 299–301. doi : 10.1016/S0140-6736(00)03623-0 . PMID 11214144 . S2CID 35896288 . ^ Dukes-Filatov disease at Who Named It?
Medication Phobia Wikipedia

Clin Dermatol . 19 (1): 69–71. doi : 10.1016/S0738-081X(00)00215-7 . PMID 11369491 . ^ "Drugs that call for extra caution. ... New York: Simon Schuster. p. 56. ISBN 978-0-684-87309-1 . ^ M.d. Kamath, Bob (30 May 2007). ... Kendall Hunt Publishing. p. 25. ISBN 978-0-7872-8701-6 . ^ Ashton CH (2002).
Lisch Epithelial Corneal Dystrophy Wikipedia

Ophthalmol. 114 (1): 35–44. doi : 10.1016/S0002-9394(14)77410-0 . PMID 1621784 . ^ Lisch W, Büttner A, Oeffner F, Böddeker I, Engel H, Lisch C, Ziegler A, Grzeschik K (October 2000). ... Ophthalmol. 130 (4): 461–8. doi : 10.1016/S0002-9394(00)00494-3 . PMID 11024418 . External links [ edit ] Classification D ICD - 10 : H18.5 OMIM : 300778 MeSH : C567588 C567588, C567588 External resources Orphanet : 98955 v t e Types of corneal dystrophy Epithelial and subepithelial Epithelial basement membrane dystrophy Gelatinous drop-like corneal dystrophy Lisch epithelial corneal dystrophy Meesmann corneal dystrophy Subepithelial mucinous corneal dystrophy Bowman's membrane Reis–Bucklers corneal dystrophy Thiel-Behnke dystrophy Stroma Congenital stromal corneal dystrophy Fleck corneal dystrophy Granular corneal dystrophy Lattice corneal dystrophy Macular corneal dystrophy Posterior amorphous corneal dystrophy Schnyder crystalline corneal dystrophy Descemet's membrane and endothelial Congenital hereditary endothelial dystrophy Fuchs' dystrophy Posterior polymorphous corneal dystrophy X-linked endothelial corneal dystrophy This article about an ophthalmic disease is a stub .
- Corneal Dystrophy, Lisch Epithelial Omim
  
  Clinical Features Lisch et al. (1992) described 5 family members and 3 unrelated patients (4 males, 4 females), aged 23 to 71 years, with bilateral or unilateral, gray, band-shaped, and feathery opacities that sometimes appeared in whorled patterns. Retroillumination showed that the opacities consisted of intraepithelial, densely crowded, clear microcysts. Light and electron microscopy disclosed diffuse vacuolization of the cytoplasm of epithelial cells in the affected area. Visual acuity was so reduced in 3 patients that abrasion of the corneal epithelium was performed. The corneal abnormalities recurred within months, with the same reduction in visual acuity as before.
- Lisch Epithelial Corneal Dystrophy Orphanet
  
  Lisch epithelial corneal dystrophy (LECD) is a very rare form of superficial corneal dystrophy characterized by feather-shaped opacities and microcysts in the corneal epithelium arranged in a band-shaped and sometimes whorled pattern, occasionally with impaired vision. Epidemiology Exact prevalence of this form of corneal dystrophy is not known but very few cases have been reported to date. LECD has been documented in one German family and in rare sporadic cases in Germany and the USA. Clinical description Lesions generally develop in childhood. Epithelial opacities are slowly progressive and painless blurred vision sometimes occurs after 60 years of age. Etiology The exact cause is unknown but appears to be genetic. The gene related to Lisch epithelial corneal dystrophy has been mapped to the short arm of the X chromosome (Xp22.3).
Charcot-Marie-Tooth Neuropathy Type 4c Gene_reviews

Foot deformities were first observed between ages two and ten years, were moderately or severely disabling, and required surgery in 6% (1/18) to 11% (3/28) of cases (Table 2). Table 2. Occurrence of Manifestations of CMT4C by Study View in own window Study Finding Study (Total Patients) Azzedine et al [2006] (28) Colomer et al [2006] (14) Senderek et al [2003] (18) Houlden et al [2009] (6) Baets et al [2011] (9) Laššuthová et al [2011] (16) Yger et al [2012] (14) Fischer et al [2012] (6) Cumulative Data Age at onset 1 st symptoms 2-10 4-39 Infancy-12 1-16 <1 1-12 1-12 ND 1-16 Neuropathy 2-10 Infancy-12 1-16 <1 2-50 2-50 2-25 1-50 Age at (last) exam (yrs) 5-45 8-45 11-56 8-42 ND ND 8-59 5-59 Foot deformity Pes cavus 20/28 14/14 1 8/18 Yes ND 13/15 12/14 ND Pes planus 7/28 4/18 Yes ND no no ND Pes valgus 1/28 ND ND ND no 3/14 ND Other No Hammer toes 8/18 Small feet ND Hammer toes no ND Total 28/28 14/14 13/18 2 6/6 1 7/9 14/15 14/14 ND 96/104 (92%) Age at onset (yrs) 2-10 No data 2-12 ND ND ND 1,12 3 ND 1-12 Surgery 3/28 None 1/13 No ND 9/14 4/14 ND 17/69 (24%) Spine deformity Total 27/28 5/14 4 11/18 4 6/6 6/9 10/12 12/12 5/6 82/105 (78%) Age at onset (yrs) 2-10 4 4-12 5 ND 2, 6, 7, 12 6 ND 7-15 ND 2-15 Surgery 7 7 + 6 8 = 13/27 1/14 1/11 3/6 3/6 ND 1/12 ND 22/76 (29%) ND = not done or not documented 1. ... Additional Clinical Findings in CMT4C by Study View in own window Clinical Finding Study (Total Patients) Azzedine et al [2006] (28) Colomer et al [2006] (14) Senderek et al [2003] (18) Houlden et al [2009] (6) Baets et al [2011] (9) Laššuthová et al [2011] (16) Yger et al [2012] (14) Cumulative Data Hypoacusis 5/28 0/14 2/18 0/6 0/9 0/15 8/13 15/103 Deafness 0/28 5/14 1/18 2/6 1/9 3/15 0/13 12/103 Nystagmus 0/28 0/14 2/18 0/6 2/9 0/15 0/13 4/103 Pupillary light reflexes 0/28 3/14 0/18 1/6 0/9 0/15 14/13 4/20 Other pupillary disturbances -- -- -- Asymmetric size 1/6 -- -- -- 1/6 Lingual fasciculation -- 3/14 -- -- -- -- -- 3/14 Tongue atrophy and/or weakness -- -- -- 1/6 -- -- 2/13 3/19 Facial paresis 1/28 -- -- 1/6 1/9 -- 4/13 7/56 Facial weakness -- -- -- 1/6 -- -- -- 1/6 Head tremor -- 2/14 -- -- -- -- -- 2/14 Vocal cord involvement -- -- -- -- -- -- 1/13 1/13 Total patients w/cranial nerve involvement 5/28 9/14 5/14 1 4/6 -- -- 10/13 33/73 Respiratory insufficiency or hypoventilation 7/28 2 -- 2/18 -- 1/9 -- -- 10/55 Sensory ataxia 1/28 2/14 -- -- -- -- -- >3/42 3 Diabetes mellitus -- -- 1/18 -- -- -- -- 1/18 Romberg sign -- 2/14 -- -- -- -- -- 2/14 1. 14 of 18 patients were examined for cranial nerve involvement. 2. ... Genotype-Phenotype Correlations Significant intrafamilial variability in the disease course makes it difficult to identify genotype-phenotype correlations [Kessali et al 1997, Gabreëls-Festen et al 1999, Senderek et al 2003, Azzedine et al 2005a, Azzedine et al 2005b, Azzedine et al 2006]. In 28 individuals with CMT4C, Azzedine et al [2006] found no correlation between the nature and the position of the pathogenic variant, disease duration, and the stage of disability.

SH3TC2, ITGA6, PMP22, SOX10, RAB11A, KIF20A
- Charcot-Marie-Tooth Disease, Type 4c Omim
  
  A number sign (#) is used with this entry because Charcot-Marie-Tooth (CMT) disease type 4C is caused by homozygous or compound heterozygous mutation in the SH3TC2 gene (608206). Mild mononeuropathy of the median nerve (MNMN; 613353) is a less severe allelic disorder caused by heterozygous mutation in the SH3TC2 gene. For a phenotypic description and a discussion of genetic heterogeneity of autosomal recessive demyelinating Charcot-Marie-Tooth disease, see CMT4A (214400). Clinical Features Kessali et al. (1997) reported 2 large consanguineous Algerian families with autosomal recessive demyelinating CMT. Mean age at onset was 5.2 years (range 2 to 10 years). All patients had foot deformities and scoliosis, often requiring surgery.
- Charcot-Marie-Tooth Disease Type 4c Orphanet
  
  Charcot-Marie-Tooth disease type 4C (CMT4C) is a subtype of Charcot-Marie-Tooth type 4 characterized by childhood or adolescent-onset of a relatively mild, demyelinating sensorimotor neuropathy that contrasts with a severe, rapidly progressing, early-onset scoliosis, and the typical CMT phenotype (i.e. distal muscle weakness and atrophy, sensory loss, and often foot deformity). A wide spectrum of nerve conduction velocities are observed and cranial nerve involvement and kyphoscoliosis have also been reported.
Acroosteolysis Wikipedia

Academia Española de Dermatología y Veneralogía. Archived from the original on 28 April 2015 . Retrieved 28 June 2014 . ^ Baran, Robert; de Berker, David A. ... Wiley. ISBN 978-0470657355 . Retrieved 28 June 2014 . ^ http://radiopaedia.org/articles/pinch-fo ^ Freedberg, et al. (2003). Fitzpatrick's Dermatology in General Medicine . (6th ed.). McGraw-Hill. ISBN 0-07-138076-0 . This condition of the skin appendages article is a stub .

NOTCH2, ZMPSTE24, LMNA, HPGD, KIF1A, CTSC, COL3A1, FLNA, PDGFRB, SCN9A, ATL3, RETREG1, IFIH1, WNK1, PTHLH, TNF
- Hajdu–cheney Syndrome Wikipedia
  
  Hajdu–Cheney syndrome Other names Acrodentoosteodysplasia, Arthrodentoosteodysplasia Hajdu-Cheney Specialty Rheumatology , medical genetics Hajdu–Cheney syndrome , also called acroosteolysis with osteoporosis and changes in skull and mandible , arthrodentoosteodysplasia and Cheney syndrome , [1] is an extremely rare autosomal dominant congenital disorder [2] [3] of the connective tissue characterized by severe and excessive bone resorption leading to osteoporosis and a wide range of other possible symptoms. Mutations in the NOTCH2 gene, identified in 2011, cause HCS. HCS is so rare that only about 50 cases have been reported worldwide since the discovery of the syndrome in 1948 [4] Contents 1 Signs and symptoms 2 Genetics 3 Pathogenesis 4 Diagnosis 4.1 Types 5 Treatment 6 Eponym 7 References 8 Further reading 9 External links Signs and symptoms [ edit ] Hajdu–Cheney syndrome causes many issues with an individual’s connective tissues. Some general characteristics of an individual with Hajdu–Cheney syndrome include bone flexibility and deformities, short stature, delayed acquisition of speech and motor skills, dolichocephalic skull, Wormian bone , small maxilla, hypoplastic frontal sinuses, basilar impression, joint laxity, bulbous finger tips and severe osteoporosis. Wormian bone occurs when extra bones appear between cranial sutures. Fetuses with Hajdu–Cheney syndrome often will not be seen to unclench their hands on obstetrical ultrasound. They may also have low-set ears and their eyes may be farther apart than on a usual child, called hypertelorism .
Cervical Polyp Wikipedia

Lippincott Williams & Wilkins. pp. 254–256. ISBN 0-7817-3905-5 . ^ a b c d e f g h i Smith, Melanie N. (2006-05-10). ... Cambridge University Press . p. 77. ISBN 1-900151-51-0 . ^ Papadakis, Maxine A.; Stephen J. ... McGraw-Hill Professional. p. 60. ISBN 0-07-145892-1 . ^ a b Bosze, Peter; David M. ... Informa Health Care. p. 66. ISBN 963-00-7356-0 . ^ "Cervical Polyps" (PDF) .

BMI1, CDKN2A, COMMD3-BMI1
Doege–potter Syndrome Wikipedia

Surg . 119 (1): 185–7. doi : 10.1016/S0022-5223(00)70242-X . PMID 10612786 . Archived from the original on 2013-01-12. ^ a b Shields, TW; LoCicero J; Ponn RB; Rusch VW (2005). ... Hagerstwon, MD: Lippincott Williams & Wilkins. pp. 893 . ISBN 0-7817-3889-X . ^ Ellorhaoui M, Graf B (February 1976). ... Hagerstwon, MD: Lippincott Williams & Wilkins. pp. 172–3 . ISBN 978-0-7817-6957-0 . v t e Paraneoplastic syndromes Endocrine Hypercalcaemia SIADH Zollinger–Ellison syndrome Cushing's syndrome Hematological Multicentric reticulohistiocytosis Nonbacterial thrombotic endocarditis Neurological Paraneoplastic cerebellar degeneration Encephalomyelitis Limbic encephalitis Opsoclonus Polymyositis Transverse myelitis Lambert–Eaton myasthenic syndrome Anti-NMDA receptor encephalitis Musculoskeletal Dermatomyositis Hypertrophic osteopathy Mucocutaneous reactive erythema Erythema gyratum repens Necrolytic migratory erythema papulosquamous Acanthosis nigricans Ichthyosis acquisita Acrokeratosis paraneoplastica of Bazex Extramammary Paget's disease Florid cutaneous papillomatosis Leser-Trélat sign Pityriasis rotunda Tripe palms Other Febrile neutrophilic dermatosis Pyoderma gangrenosum Paraneoplastic pemphigus v t e Tumours of endocrine glands Pancreas Pancreatic cancer Pancreatic neuroendocrine tumor α : Glucagonoma β : Insulinoma δ : Somatostatinoma G : Gastrinoma VIPoma Pituitary Pituitary adenoma : Prolactinoma ACTH-secreting pituitary adenoma GH-secreting pituitary adenoma Craniopharyngioma Pituicytoma Thyroid Thyroid cancer (malignant): epithelial-cell carcinoma Papillary Follicular / Hurthle cell Parafollicular cell Medullary Anaplastic Lymphoma Squamous-cell carcinoma Benign Thyroid adenoma Struma ovarii Adrenal tumor Cortex Adrenocortical adenoma Adrenocortical carcinoma Medulla Pheochromocytoma Neuroblastoma Paraganglioma Parathyroid Parathyroid neoplasm Adenoma Carcinoma Pineal gland Pinealoma Pinealoblastoma Pineocytoma MEN 1 2A 2B
Angina Wikipedia

Retrieved April 28, 2010 . ^ Kaski (editor), Juan Carlos (1999). ... New York: McGraw-Hill. p. 140 . ISBN 978-0-07-148501-2 . ^ "Health Benefits of Cessation" . ... Pathophysiology of Disease: An Introduction to Clinical Medicine (6th ed.). p. 276. ISBN 978-0-07-162167-0 . ^ Thomas, Michel (2005-09-13). ... ISBN 978-0071422802 . ^ Podrid, Philip J (November 28, 2012). "Pathophysiology and clinical presentation of ischemic chest pain" . ... Drug discovery: a history . ISBN 978-0-471-89980-8 . [ page needed ] ^ Sulfi, S.; Timmis, A.

AVP, PLAU, APOE, LDLR, GLA, CRELD1, ABCG8, ABCG5, GATA4, GATA6, XYLT2, XYLT1, NR2F2, LMNA, LCAT, JAK2, HLA-DPA1, HLA-DPB1, LDLRAP1, IDUA, LIPC, CYP27A1, TET2, PRTN3, ZMPSTE24, CTLA4, SCN5A, PTEN, MPL, ENPP1, PIGA, PCSK9, PTPN22, ABCC6, VEGFA, PMM2, APOB, ACE, CRP, CAD, CCS, IL6, SERPINE1, ITGB2, TNNI3, DLD, CXCL16, OXCT1, LAD1, SERPINA5, PLA2G1B, APOA1, TNF, NOS3, PLB1, KLF14, PLA2G7, PLA2G6, YWHAZ, IL37, NEAT1, VIP, MIR208A, MIR34A, MIR499A, TNFRSF1B, ZGLP1, CYP4F2, PROM1, TNFSF10, CPSF4, HDL3, MOCOS, QRSL1, POC1A, TBC1D9, JTB, ZC4H2, CMAS, SELL, EHMT1, PPP1R2C, FERMT3, ADIPOQ, WASF1, NLRP3, NR1I2, FGF21, ADAM10, CCL2, EDN1, ICAM1, HSPA5, GNB3, GLP1R, GLB1, GDF10, GCG, FGF4, F5, F3, CYP19A1, RENBP, CPB2, CLCN1, CETP, CD34, CD14, VPS51, KLK3, APOC3, ALB, AGTR1, IFNG, IGF2R, IL1A, IL1B, PYGM, PRKCD, PLXNA2, PLA2G2A, ABCB1, PAPPA, CNTN3, ADRB1, OPA1, NOS2, NOS1, MPI, MMP3, SMCP, LPA, KDR, ITGA2B, IL10, CXCL8, IL7, IL1RN, LINC02605
- Angina Mayo_clinic
  
  Overview Angina (an-JIE-nuh or AN-juh-nuh) is a type of chest pain caused by reduced blood flow to the heart. Angina is a symptom of coronary artery disease. Angina is also called angina pectoris. Angina pain is often described as squeezing, pressure, heaviness, tightness or pain in the chest. It may feel like a heavy weight lying on the chest. Angina may be a new pain that needs to be checked by a health care provider, or recurring pain that goes away with treatment. Although angina is relatively common, it can still be hard to distinguish from other types of chest pain, such as the discomfort of indigestion.
Juvenile Myoclonic Epilepsy Wikipedia

"Epidemiology of juvenile myoclonic epilepsy". Epilepsy Behav . 28 Suppl. 1: S15–17. doi : 10.1016/j.yebeh.2012.06.024 . ... "Chronodependency and provocative factors in juvenile myoclonic epilepsy". Epilepsy Behav . 28 Suppl 1: S25-9. doi : 10.1016/j.yebeh.2012.11.045 . ... "The quest for juvenile myoclonic epilepsy genes". Epilepsy Behav . 28 Suppl 1: S52-7. doi : 10.1016/j.yebeh.2012.06.033 . ... Cell . 88 (3): 385–392. doi : 10.1016/S0092-8674(00)81877-2 . ^ Escayg, A; De Waard, M; Lee, DD; Bichet, D; Wolf, P; Mayer, T; Johnston, J; Baloh, R; Sander, T; Meisler, MH (2000). ... Progress in Brain Research. 213 : 55–85. doi : 10.1016/B978-0-444-63326-2.00003-X . ISBN 9780444633262 .

EFHC1, GABRA1, CACNB4, JRK, KCNQ3, CLCN2, GABRD, CILK1, BRD2, CTF1, CHRNA4, EJM2, GABRG2, GJD2, GRM4, SCN1A, CSTB, GABRB3, SEC14L2, ME2, CHRNA7, KCNQ2, KCND3, TRPM2, IGHE, TAP1, EFHC2, GJA8, GABBR1, REM1, RMDN1, PADI4, LGSN, BCL9, SLC12A5, RMDN3, LRRC1, SYBU, CPA6, CLOCK, MMEL1, DHX40, NPL, CHRFAM7A, RBM45, RMDN2, MED19, SLC12A6, SELENOP, ABCG2, KCNJ3, CASR, DNMT1, ATN1, EXT1, F2, GABRA5, HLA-DPB1, HLA-DQA1, HLA-DRB1, HLA-F, KCNJ6, TOP3B, CFP, ABCB1, PLXNB1, HCN2, SLC6A4, SLC12A2, TFAP2B, ALDH5A1, PER3, PER2, STIN2-VNTR
- Epilepsy, Idiopathic Generalized, Susceptibility To, 13 Omim
  
  A number sign (#) is used with this entry because of evidence that susceptibility to idiopathic generalized epilepsy-13 (EIG13), including juvenile myoclonic epilepsy-5 (EJM5) and childhood absence epilepsy-4 (ECA4), can be conferred by heterozygous mutation in the GABRA1 gene (137160) on chromosome 5q34. Description Childhood absence epilepsy and juvenile myoclonic epilepsy are both subtypes of what has classically been called idiopathic generalized epilepsy (IGE, EIG; see 600669). For a phenotypic description and a discussion of genetic heterogeneity of idiopathic generalized epilepsy, see 600669. For a phenotypic description and a discussion of genetic heterogeneity of juvenile myoclonic epilepsy and childhood absence epilepsy, see ECA1 (600131) and JME (254770), respectively. Clinical Features Cossette et al. (2002) reported a French Canadian family in which 14 members over 4 generations had juvenile myoclonic epilepsy.
- Epilepsy, Idiopathic Generalized, Susceptibility To, 7 Omim
  
  For a phenotypic description and a discussion of genetic heterogeneity of idiopathic generalized epilepsy (IGE), see 600669. Juvenile myoclonic epilepsy (JME; see 254770) is a form of idiopathic generalized epilepsy. Mapping Elmslie et al. (1997) tested for linkage between JME and chromosomal regions harboring genes for nAChR subunits in 34 pedigrees using parametric and nonparametric analyses. Strong evidence for linkage with heterogeneity was found to polymorphic loci encompassing the region containing the gene that encodes the alpha-7 subunit of nAChR (CHRNA7; 118511), which maps to chromosome 15q14. Elmslie et al. (1997) suggested that this major locus (EJM2) contributes to genetic susceptibility to JME in a majority of the families studied.
- Juvenile Myoclonic Epilepsy Orphanet
  
  Juvenile myoclonic epilepsy is the most common hereditary idiopathic generalized epilepsy syndrome and is characterized by myoclonic jerks of the upper limbs on awakening, generalized tonic-clonic seizures manifesting during adolescence and triggered by sleep deprivation, alcohol intake, and cognitive activities, and typical absence seizures (30% of cases).
- Myoclonic Epilepsy, Juvenile, Susceptibility To, 4 Omim
  
  For a phenotypic description and a discussion of genetic heterogeneity of juvenile myoclonic epilepsy (JME), see 254770. JME is a form of idiopathic generalized epilepsy (IGE; 600669). Clinical Features Kapoor et al. (2007) reported a family from southern India in which 8 individuals had juvenile myoclonic epilepsy inherited in an autosomal dominant pattern. The proband was a 32-year-old woman who developed morning myoclonic jerks at age 14 years and generalized tonic-clonic seizures at age 20. EEG recordings showed polyspike and wave discharges characteristic of a generalized epilepsy. Other affected members had a similar history. None had absence or febrile seizures.
- Juvenile Myoclonic Epilepsy Gard
  
  Juvenile myoclonic epilepsy is an epilepsy syndrome characterized by myoclonic jerks (quick jerks of the arms or legs), generalized tonic-clonic seizures (GTCSs), and sometimes, absence seizures . The seizures of juvenile myoclonic epilepsy often occur when people first awaken in the morning. Seizures can be triggered by lack of sleep, extreme fatigue, stress, or alcohol consumption. Onset typically occurs around adolesence in otherwise healthy children. The causes of juvenile myoclonic epilepsy are very complex and not completely understood.
- Epilepsy, Juvenile Myoclonic, Susceptibility To, 10 Omim
  
  A number sign (#) is used with this entry because of evidence that susceptibility to juvenile myoclonic epilepsy-10 (EJM10) is conferred by heterozygous mutation in the ICK gene (612325) on chromosome 6p12. Description Juvenile myoclonic epilepsy-10 is an autosomal dominant seizure disorder with variable manifestations, even within families. Affected individuals have febrile, myoclonic, tonic-clonic, or absence seizures, although several seizure types can occur in the same individual. The age of onset also shows great variability: some patients present in the first years of life, whereas other have onset of seizures in teenage years. EEG typically shows 3.5 to 5 Hz polyspike wave discharges. There is evidence of incomplete penetrance (summary by Bailey et al., 2018).
- Epilepsy, Juvenile Myoclonic, Susceptibility To, 9 Omim
  
  For general phenotypic information and a discussion of genetic heterogeneity of juvenile myoclonic epilepsy, see 254770. Clinical Features Ratnapriya et al. (2010) reported a 4-generation family from southern India in which 6 living members had juvenile myoclonic epilepsy. Age at onset ranged from 12 to 20 years, and all had myoclonic seizures with secondary generalized tonic-clonic seizures. Two patients had a history of febrile seizures, and 2 had absence seizures. EEG showed generalized 4-6 Hz polyspike and wave discharges characteristic of a generalized epilepsy.
- Epilepsy, Idiopathic Generalized, Susceptibility To, 11 Omim
  
  A number sign (#) is used with this entry because some evidence has suggested that susceptibility to idiopathic generalized epilepsy-11 (EIG11), juvenile myoclonic epilepsy-8 (EJM8), and juvenile absence epilepsy-2 (EJA2) may be conferred by variation in the chloride channel-2 gene (CLCN2; 600570) on chromosome 3q27. However, there has been some controversy over whether variation in the CLCN2 gene has a role in epilepsy (see MOLECULAR GENETICS). Description Both juvenile myoclonic epilepsy and juvenile absence epilepsy are subtypes of idiopathic generalized epilepsy (EIG). For a general phenotypic description and a discussion of genetic heterogeneity of these disorders, see EIG (600669), EJM (254770), and EJA (607631). Mapping Sander et al. (2000) used nonparametric multipoint linkage analysis to identify susceptibility loci among 130 IGE-multiplex families ascertained through a proband with childhood or juvenile absence epilepsy or juvenile myoclonic epilepsy, and 1 or more sibs affected by an IGE trait.
- Epilepsy, Idiopathic Generalized, Susceptibility To, 9 Omim
  
  A number sign (#) is used with this entry because of evidence that susceptibility to idiopathic generalized epilepsy-9 (EIG9) and juvenile myoclonic epilepsy-6 (EJM6) is conferred by mutation in the CACNB4 gene (601949) on chromosome 2q23. Description For a general phenotypic description and a discussion of genetic heterogeneity of idiopathic generalized epilepsy, see 600669. Juvenile myoclonic epilepsy is a subtype of idiopathic generalized epilepsy; see 254770 for a general phenotypic description and a discussion of genetic heterogeneity of JME. Clinical Features Escayg et al. (2000) reported a woman with a history of sporadic typical absence seizures (brief spells of loss of consciousness) and repetitive bilateral myoclonic jerks in the shoulders and arms after awakening, since age 9 years. She never had loss of consciousness. Her epilepsy syndrome was classified as juvenile myoclonic epilepsy.
- Myoclonic Epilepsy, Juvenile, Susceptibility To, 3 Omim
  
  For general phenotypic information and a discussion of genetic heterogeneity of juvenile myoclonic epilepsy, see 254770. Mapping Greenberg et al. (1987) studied 24 families with JME. Segregation analysis allowed them to reject fully penetrant dominant and recessive models. For the linkage analysis, they assumed a fully penetrant recessive model or a recessive model with 60% penetrance. Using either clinical phenotype or EEG changes to score persons as affected with JME, Greenberg et al. (1987, 1988) found evidence for linkage to BF (138470) and HLA (142800) on chromosome 6p21; the lod score exceeded 3.0 when HLA and BF were used together. Greenberg et al. (1989) and Delgado-Escueta et al. (1989) presented additional evidence for linkage to HLA and BF.
- Epilepsy, Myoclonic Juvenile Omim
  
  A number sign (#) is used with this entry because of evidence that susceptibility to juvenile myoclonic epilepsy-1 (EJM1) is conferred by variation in the EFHC1 gene (608815) on chromosome 6p12. See also susceptibility to juvenile absence epilepsy (JAE, EAJ; 607631), which is also conferred by variation in the EFHC1 gene. Description Juvenile myoclonic epilepsy is a subtype of idiopathic generalized epilepsy (EIG; see 600669) affecting up to 26% of all individuals with EIG. Individuals with JME have afebrile seizures only, with onset in adolescence of myoclonic jerks. Myoclonic jerks occur usually in the morning (Janz and Durner, 1997).
- Epilepsy, Idiopathic Generalized, Susceptibility To, 10 Omim
  
  A number sign (#) is used with this entry because of evidence that susceptibility to idiopathic generalized epilepsy-10 (EIG10), generalized epilepsy with febrile seizures plus, type 5 (GEFSP5), and juvenile myoclonic epilepsy-7 (EJM7) can be conferred by variation in the GABRD gene (137163) on chromosome 1p36.3. Description Idiopathic generalized epilepsy (EIG) is a broad term that encompasses several common seizure phenotypes, classically including childhood absence epilepsy (CAE, ECA), juvenile absence epilepsy (JAE), and juvenile myoclonic epilepsy (JME, EJM) (Commission on Classification and Terminology of the International League Against Epilepsy, 1989). Generalized epilepsy with febrile seizures plus (GEFS+) shows phenotypic overlap with IGE, and includes patients with early-onset febrile seizures who later develop various types of febrile and afebrile seizures, such as those observed in EIG (summary by Singh et al., 1999). For a general phenotypic description and a discussion of genetic heterogeneity of EIG, see 600669. For a general phenotypic description and a discussion of genetic heterogeneity of GEFS+, see 604233.
Nosocomephobia Wikipedia

Oxford University Press . ISBN 978-0-19-852783-1 . ^ Glenn, Harrold. "The Ultimate Self-Hypnosis Cure for the Phobia of Hospitals (Nosocomephobia)" . ... Archived from the original on 1 October 2015 . Retrieved 28 November 2009 . ^ "Doctor Tells Nixon's Fear of Hospital" . ... Toledo Blade. September 15, 1974 . Retrieved 28 November 2009 . [ dead link ] ^ νοσοκομεῖον , Henry George Liddell, Robert Scott, A Greek-English Lexicon , on Perseus ^ φόβος , Henry George Liddell, Robert Scott, A Greek-English Lexicon , on Perseus ^ Thomas, Charles (2001). ... University of Michigan : Charles C. Thomas. ISBN 0-398-07132-2 . This abnormal psychology –related article is a stub .
Odynophagia Wikipedia

Houghton Mifflin Company . Retrieved 28 February 2017 . ^ "Medical Definition of Odynophagia" . MedicineNet . 13 May 2016 . Retrieved 28 February 2017 . ^ a b Schiff, Bradley A. ... Merck Sharp & Dohme Corp . Retrieved 28 February 2017 . ^ Allan B. Wolfson, ed. (2005). Harwood-Nuss' Clinical Practice of Emergency Medicine (4th ed.). pp. 307–8. ISBN 0-7817-5125-X . ^ Scully, Crispian (2008). ... Edinburgh: Churchill Livingstone. pp. 131–139. ISBN 978-0-443-06818-8 . ^ Mayo Clinic Staff (8 August 2016).

CRP, NT5E