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Office hours Wednesday 3-4pm 304A Stanley Hall Review session 5pm Thursday, Dec. 11 GPB100.

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Presentation on theme: "Office hours Wednesday 3-4pm 304A Stanley Hall Review session 5pm Thursday, Dec. 11 GPB100."— Presentation transcript:

1 Office hours Wednesday 3-4pm 304A Stanley Hall Review session 5pm Thursday, Dec. 11 GPB100

2 Coding sequence array Fig. 1.13

3 “RNA-seq” AAAAA counts seqmapsgenome pos orient 26982 TCGTTCACTTGTATTGG U0 sbaySum.fsa 3002121R 25885 TCTCTACTGGTGGTGGT U0 chr03.fsa 138912 F 17851 GACAAACTGTCGCTGTC R0 15715 TCTCTACCGGTGGTGGT U0 sbaySum.fsa 11182634F 14963 TCGTTCACTTGTAATGG U0 chr04.fsa 1489376R … 610 TTGAAGCTACCACCAAC R0 607 TGTCCTTATCTATGTGT U0 sbaySum.fsa 8491512 R 602 CGTACTTTTTTAATTGT U1 chr11.fsa 145622 F 602 ATCATTGTTCCAGAAAT R0 601 TTATCAGAGGTGCTGGT U0 chr14.fsa 694435 R 600 CAAAGACCTCATTTAAT U0 sbaySum.fsa 4671591 R 599 AGGAGGGTATATATGCT U0 chr14.fsa 575509 R … Solexa sequencing

4 Expression effects of cancer

5 Diagnosis via transcriptional profile transcripts patient samples

6 Diagnosis via transcriptional profile

7 Linkage mapping of mRNA levels “Black 6” mousex“DBA” mouse 111 F 2 progeny Microarray each F 2 liver … Genotype each F 2 Looking for linkage (coinheritance) between marker and mRNA level.

8 Marker is linked to polymorphism in expression regulation cascade ORF TF G kinase TF G G

9 Locally acting polymorphisms Polymorphism responsible for mRNA difference is at the locus of the gene itself ~25% of varying mRNAs are caused by locally acting polymorphism

10 Nonlocal polymorphisms

11 One polymorphism in a key regulator can affect a regulon: 100’s of related mRNAs.

12 Clinical applications “Black 6” mousex“DBA” mouse 111 F 2 progeny Microarray each F 2 liver … Genotype each F 2 Measure fat pad each F 2

13 Clinical applications

14 Colored curves = fat mass at different body locations

15 Clinical applications Finding polymorphism responsible for difference in macroscopic phenotype is hard

16 Clinical applications Finding polymorphism responsible for difference in macroscopic phenotype is hard If mRNAs change too, can learn mechanism from known function of encoded proteins

17 Clinical applications

18

19

20 Counts allele 1/allele 2, cases Counts allele 1/allele 2, controls = 1.5

21 Clinical applications

22 Marker predicts quantitative expression level = association

23 Can we map expression traits first, disease afterward?

24 Linkage of human transcripts

25

26 Association of human transcripts

27 linkage (families) assoc (unrelated)

28 Association in multiple populations Han Chinese and Japanese European-Americans in Utah

29 Association in multiple populations

30 A new brand of genetic variation

31 Fig. 8.25 Translation

32 Fig. 8.25 Translation

33 PSI+ yeast read through STOPs

34

35 40-150 bp

36 Weird genetics of read-through Haploid PSI+ Haploid psi- Diploid PSI+

37 Weird genetics of read-through Haploid PSI+ Haploid psi- Diploid PSI+ sporulate Haploid PSI+ …

38 Weird genetics of read-through Haploid PSI+ Haploid psi- Diploid PSI+ sporulate Haploid PSI+ But why wouldn’t it get diluted over many divisions?

39 Cytoplasmic aggregates of Sup35

40 How would this explain the results? Cytoplasmic aggregates of Sup35

41 Hard to make aggregate, easy to join

42 Protein inheritance

43 Original from PSI+ nucleates in all progeny

44 PSI+ begets more PSI+ Not due to dominant genetics in the usual way.

45 Nucleating prions in mad cow disease

46 Is PSI+ the yeast analog of mad cow or Alzheimer’s?

47 If bad, would be lost

48 (Pichia methanolica vs. S. cerevisiae)

49 PSI+ phenotypes

50 Genetically distinct S. cerevisiae strains

51 PSI+ phenotypes Genetically distinct S. cerevisiae strains

52 PSI+ phenotypes 50°C Genetically distinct S. cerevisiae strains

53 PSI+ phenotypes 50°C Genetically distinct S. cerevisiae strains

54 PSI+ phenotypes Why would aggregates result in so many novel abilities and traits??

55 PSI+ phenotypes Why would aggregates result in so many novel abilities and traits?? Apparently does not happen in Alzheimer’s…

56 The clincher

57 (partial LOF)

58 The clincher (partial LOF) What do you conclude? A.Sup35 does not cause resistance to paraquat. B.Prions do not cause resistance to paraquat. C.Aggregation is not necessary to cause resistance to paraquat. D.Aggregation is not sufficient to cause resistance to paraquat.

59 The clincher (partial LOF) Aggregates per se don’t cause resistance.

60 The clincher (partial LOF) Aggregates per se don’t cause resistance. Losing function of sup35 does.

61 Aggregation = more read-through

62 New extra-long forms of proteins cause new traits.

63 PSI+ allows epigenetic change in protein sequence.

64 Genetic effects? Phenotypes varied between genetically diverse PSI+ strains. Genetically distinct S. cerevisiae strains

65 Genetic effects? Phenotypes varied between genetically diverse PSI+ strains. How can the cause be genetic and non-genetic (protein aggregates) at the same time? Genetically distinct S. cerevisiae strains

66 Aggregation = more read-through

67 UTR mutations usually occur and have no effect

68 Aggregation = more read-through UTR mutations usually occur and have no effect, so organism doesn’t die and allele is maintained.

69 Aggregation = more read-through UTR mutations usually occur and have no effect, so organism doesn’t die and allele is maintained. Now in PSI+, they manifest!

70 Aggregation = more read-through Sequence differences in read- through region cause phenotypic differences between PSI+ strains.

71 Cryptic variation: DNA sequence differences between individuals that are usually not expressed

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