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Sex Chromosomes and inheritance X-Linked Traits 1 Sutton’s Hypothesis Genes are structures localized on chromosomes Each of the two alleles is on one chromosome of a couple of chromosomes 2 Each allele of a gene is located on one chromosome of a couple. At the end of meiosis each gamete contains only one allele of each gene. If two genes (4 alleles ) are considered we can observe independent segregation of the alleles of the two genes (Mendel’s 3rd law) 4 Chromosomal sex determination Insect, protenor belfragei (Stevens, 1900) FEMALE MALE 14 CHROMOSOMES 13 7 BIVALENTI 6 + 1 GAMETES [F >>7] [M>>6] [M>>7] 7 + 7 = 14 FEMALE XX 7 + 6 = 13 MALE X0 5 6 HUMAN KARYOTYPE 7 Sex and Chromosomes FEMALE MALE XX XY BIRDS, SOME REPTILES ZW ZZ 8 In some species environmental factors are relevant for sex determination 9 HUMAN KARYOTYPE 10 zanzara Meiotic pairing between X and topo Y is at terminal regions called pseudo-autosomal renna marmotta hamster cinese 11 DIAKINESIS IN MAN 12 Homologous regions between X and Y: pseudo autosomal region Testis Determining Factor=TDF (sex determinig region Y) TDF = SRY 13 Female : XX >> X+X+ X+X XX Male XY >> X+Y XY Drosophila Melanogaster 15 Inheritance of X‐linked Gene for Eye Colour in Drosophila The first X‐linked gene found in Drosophila was the recessive white eye mutation (Morgan, 1910). When a homozygous red‐eyed female (dominant) is crossed with a white‐eyed male (recessive), all individuals in the F1 are red‐eyed. X* White (r) Y X Red (D) X X* XY X Red (D) X X* XY 17 When we cross the individuals from F1……… X Red (D) Y X Red (D) XX XY X* White (r) XX* X*Y 18 …but when the cross is between a white‐eyed female and red‐eyed male, male offspring in the F1 have white eyes. X Red (D) Y X* White (r) XX* X*Y X* XX* X*Y 19 When heterozygous red eyed females are crossed with white‐ eyed males, both sexes segregate 1: 1 X* White (r) Y X* X*X* X*Y X Red (D) XX* XY 20 These experiments demonstrate that eye color gene in this case is carried by the X chromosome, but not by the Y. X-Linked Recessive Diseases 22 X-Linked Recessive Disease Rare Gene: Haemofilia 2:10.000 no male to male transmission 23 Haemophilia in old ages Circumcision 24 Pedigree showing inheritance of hemophilia, an X‐linked trait, in the descendants of Queen Victoria. Many of the descendants in the third and fourth generations (third and fourth rows) have been omitted because the mutant gene was not transmitted to them. Daltonism Normal reads: 74 Daltonic reads: 21 26 X-Linked Recessive Disease Common Allele G6PDH Deficiency VICIA FABA 27 Some drugs can cause haemolysis in GSPDH deficient subjects this peripheral smear of RBCs shows Heinz bodies. Heinz bodies are precipitated, oxidized hemoglobin. They are found in glucose‐6‐phosphate dehydrogenase deficiency (G6PD). 310200 MUSCULAR DYSTROPHY, DUCHENNE TYPE; DMD Gene map locus Xp21.2 310200 MUSCULAR DYSTROPHY, DUCHENNE TYPE; DMD Gene map locus Xp21.2 a | In Duchenne muscular dystrophy (DMD) patients, with a deletion of exons 45–54, an out‐of‐ frame transcript is generated in which exon 44 is spliced to exon 55. Owing to the frame shift, a stop codon occurs in exon 55, which prematurely aborts dystrophin synthesis. b | Using an exon‐internal antisense oligonucleotide (AON) in exon 44, the skipping of this exon can be induced in cultured muscle cells. Accordingly, the transcript is back in‐frame and a Becker muscular dystrophy (BMD)‐like dystrophin can be synthesized Fabry disease: symptoms in carriers: Late onset of symtoms. MacDermot et al. (2001) reported clinical manifestations and impact of disease in 60 females with Fabry disease. The median cumulative survival was 70 years, representing an approximate reduction of 15 years from the general population. Six of 32 women had renal failure, 9 of 32 (28%) died of cerebrovascular complications, and 42 (70%) had experienced neuropathic pain. Twenty (30%) female patients had some serious or debilitating manifestation of Fabry disease. X-Linked Dominant Diseases •Females are affected twice as males •Affected males transmit the disease to all daughters but to no sons 34 #300049 HETEROTOPIA, PERIVENTRICULAR, X‐LINKED DOMINANT Alternative titles; symbols HETEROTOPIA, FAMILIAL NODULAR PERIVENTRICULAR NODULAR HETEROTOPIA 1; PVNH1 HETEROTOPIA, PERIVENTRICULAR NODULAR, WITH FRONTOMETAPHYSEAL DYSPLASIA, INCLUDED Gene map locus Xq28 TEXT A number sign (#) is used with this entry because X‐linked periventricular heterotopia is caused by mutation in the gene encoding filamin‐A (FLNA; 300017). DESCRIPTION Periventricular heterotopia (PVNH) is a genetically heterogeneous condition. See also PVNH2 (608097), PVNH3 (608098), PVNH4 (300537), and PVNH5 (612881) If we know that the child is affected with an X‐linked disease, than we can deduct the genotypes. Be aware of exceptions! Fragile X Syndrome • Second most common cause of mental retardation (after Down syndrome) • Cytogenetic abnormality appears as a constriction in the long arm of X‐chromosome during folate deficient culture conditions • Mutation is present in an untranslated portion of the Familial Mental Retardation Gene (FMR‐1) • Loss of function mutation Fragile-X Downloaded from: Robbins & Cotran Pathologic Basis of Disease (on 18 July 2005 09:03 PM) © 2005 Elsevier Fragile X Transmission • Male carrier – detected by pedigree analysis and genetic tests – 20% are clinically and cytogenetically normal • Daughters are obligate carriers – 50% are affected (i.e. retarded) – transmit disease to grandsons of male carrier • Risk of phenotypic effects – depends on position in pedigree – Sherman paradox • Anticipation – defect worsens with each successive generation Fragile-X Pedigree Downloaded from: Robbins & Cotran Pathologic Basis of Disease (on 18 July 2005 09:03 PM) © 2005 Elsevier Fragile X Diagnosis • Cytogenetics • PCR based molecular methods of repeats in FMR‐1 gene – normal – 10 ‐55 repeats – permutation – 55‐200 repeats in carrier state – mutation – 200 ‐ 4000 in full clinical syndrome • Affected females – unfavorable lyonization Genetic and phenotypic heterogeneity A B * * C * D E * * A-E: different genes Same phenotype * mutation Different phenotypes * * * * * One gene, different mutations * Same phenotype * * Different phenotypes Same phenotype One gene, identical mutations
