Pathophysiology 101-823

1. Pathophysiology 101-823 Unit 2Genetics & Genetic DiseaseMolecular Genetics & The Genetic Control Of Proteins Paul Anderson Fall 2008

2. Nucleotides - 1 DNA and RNA are NUCLEIC ACIDS(or POLYNUCLEOTIDES) i.e. POLYMERS made up of MONOMERS called NUCLEOTIDES. Each NUCLEOTIDE has 3 parts, a 5 C or PENTOSE SUGAR, a P containing PHOSPHATE group and a N containing (NITROGENOUS)BASE. The PENTOSE SUGAR in nucleotides of DNA is DEOXYRIBOSE while in RNA, ATP, ADP or AMP it is RIBOSE. The N - containing BASE can be a single ring structure, called a PYRIMIDINE (bases CYTOSINE,THYMINE or URACIL) or a double ring structure, called a PURINE (e.g. ADENINE or GUANINE).

3. Nucleotides - 2

4. Nucleotides - 3 In each nucleotide the N base is bonded to carbon 1’ of the pentose while the phosphate group is bonded to carbon 5’ of the same sugar. components of a nucleotide

5. DNA Nucleotides DNAis a DOUBLE POLYNUCLEOTIDE STRAND containing the bases ADENINE (A), GUANINE (G), CYTOSINE (C) and THYMINE (T). DeoxyRibose

6. RNA Nucleotides RNAis a SINGLE POLYNUCLEOTIDE STRAND, containing the same bases as in DNA, except that THYMINE (T) is replaced by URACIL (U). U replaces T Ribose

7. Mononucleotides Single NUCLEOTIDES are called MONONUCLEOTIDES and include AMP composed of RIBOSE, ADENINE and a PHOSPHATE group. N base Pentose

8. Nucleic Acids - 1 NUCLEOTIDES join together to form a POLYNUCLEOTIDE strand by bonding between the PENTOSE SUGAR of one nucleotide and the PHOSPHATE group of another. Since each sugar and each phosphate form 2 bonds between the HYDROXYL (ALCOHOL) group of the sugar and the ACIDICPHOSPHATEthese two ester linkages together form a PHOSPHO – DIESTER LINKAGE. In the phosphodiester linkage each PHOSPHATE group is bonded to carbon 5’ of one sugar and to carbon 3’ of another sugar. The "BACKBONE " of a POLYNUCLEOTIDE is thus composed of SUGARS and PHOSPHATES joined by PHOSPHO – DIESTERlinkages while the N BASES project sideways from sugars.

9. Nucleic Acids - 2 P Phosphodiester linkage P P P Fig. 5.26 Campbell & Reece

10. Nucleic Acids - 3 Each POLYNUCLEOTIDE has a distinct polarity, with a “free-OH” group on C 3’ and a 5’ end which contains the terminal PHOSPHATE. Elongation of a polynucleotide normally occurs by adding new nucleotides to the 3’ end so the chain elongates in a 5’----> 3’ direction. Direction of growth 5’-----------> 3’

11. DNA Structure DNA is a DOUBLE POLYNUCLEOTIDE STRAND containing the bases ADENINE (A),THYMINE (T),CYTOSINE (C) and GUANINE (G). In any polynucleotide the percentage of PURINE BASES equals the percentage of PYRIMIDINE BASES. Also % ADENINE = % THYMINEand % CYTOSINE = % GUANINE. Watson & Crickproposed (in 1953) that the 2 polynucleotide strands of DNA are coiled around each other into a into a DOUBLE HELIX with the N BASES connecting the two strands, like the rungs of a spiral staircase with the SUGARSand PHOSPHATESforming the sides

12. DNA Structure - 2: Base Pair Rule According to the Watson - Crick model of DNA the 2 polynucleotide strands of DNA are connected by HYDROGEN BONDS formed between theN BASES of each strand, ADENINE always pairing with THYMINE (each of which can form 2 H bonds) and GUANINE with CYTOSINE(each of which forms 3 H bonds). This pattern of base pairing is called the BASE PAIR RULE. Each base is said to be COMPLEMENTARY to its partner, thus ADENINEis complementary to THYMINE and GUANINE is complementary to CYTOSINE. PURINE with PYRIMIDINE BASE A with T PAIR G with C RULE

13. DNA Double Helix 3’ end 5’ end

14. DNA Structure - 3 The 2 DNA strands are notidentical. Each polynucleotide strand contains a set of bases COMPLEMENTARY to that of the other strand. According to the Watson - Crick model the two DNA strands are "ANTIPARALLEL" i.e. if one strand is 3’<---- 5' the other strand is 5’------>3'. If one DNA strand has the base sequence 5'TAAGCT3' its complementary DNA strand will have the sequence 3’ ATTCGA 5’. H bonds Antiparallel DNA Strands

15. The Genetic Code The function of the DNA molecule is to contain the GENETIC INFORMATION for the organism (i.e. information for making all PROTEINmolecules). ALL GENETIC INFORMATION for the organism must be coded somehow in the structure of DNA. This code is called the GENETICCODE. The GENETIC CODE is thus coded information in the molecular structure of DNAfor making PROTEIN molecules. The SUGAR and PHOSPHATE groups in each DNA nucleotide are always the same and therefore could not provide a code for PROTEINS which are composed of 20 different AMINO ACIDS. The GENETIC CODE must therefore be in the only variable part of DNA, the NITROGEN BASES.

16. The Genetic Code - 2 Only by using TRIPLET combinations of the four bases A, T, G and C could we form enough CODE "WORDS" (or CODONS) for the 20 different AMINO ACID building blocks in PROTEINS. Code word (triplet of bases) corresponds to specific amino acid

17. The Genetic Code - 3 Watson & Crick proposed (in 1953) that the GENETIC CODE consists of a SPECIFIC TRIPLET of BASES of NUCLEOTIDES (each specific triplet forming a code word (or CODON) along one of the two DNA strands.

18. The Genetic Code - 4 Most GENES consist of a series of CODONS corresponding to the specific NUMBER, TYPE, and SEQUENCE of AMINO ACIDSin the PROTEIN controlled by that gene. Therefore, the GENE dictates the STRUCTURE of the PROTEIN it controls. A GENE which codes for a PROTEIN of 100 AMINO ACIDS would need to be at least 100CODONS in length, i.e. contain at least 300BASES.

19. Relationship Between DNA and Protein Primary Structure of Protein (number, type & sequence of amino acids) determines Primary Structure of Gene (number, type & sequence of codons)

20. Protein Synthesis: Transcription DNAis the molecule which stores the GENETIC CODE but since DNA never leaves the nucleus whereas protein synthesis occurs in the cytoplasm the information for making a protein must be conveyed from the nucleus to the cytoplasm by another molecule calledmessengerRNAor mRNA. A molecule of mRNA is synthesised by base pairing between single mRNA nucleotides and DNA nucleotides from one DNA strand. This is the same as base pairing in DNA except that Adenine (A) in DNA base pairs withURACIL (U) in mRNA(instead ofTHYMINE (T).

21. Transcription - 2 DNA codons Requires RNA polymerase mRNA codons

22. Transcription & Function of mRNA • After base pairing occurs, the free nucleotides are joined together (i.e. polymerise) to form an mRNA molecule. Formation of mRNA is calledTRANSCRIPTIONof the GENETIC CODE since the code is simply transferred (or transcribed) from theDNA molecule tomRNAusing the enzyme RNA Polymerase. The newly formed mRNA molecule is complementary to the DNA strand from which it was formed. • The function of mRNA is to receive GENETIC INFORMATION from one GENE in DNA and to carry this messageout of the nucleus to the sites for protein synthesis (RIBOSOMES) in the cytoplasm. • mRNA carries the GENETIC CODE in the form of a series of mRNA CODONS out of the nucleus to a ribosome particle.

23. Overview of Protein Synthesis Transcription Translation

24. Translation - 1 • tRNAmolecules bring AMINO ACIDS to the ribosome one by one. Each tRNA molecule has a triplet of bases (anANTICODON) which can base pair with a specific mRNA CODON. In this way tRNA molecules arrive in an order dictated by the order of codons in mRNA i.e. by the GENETICCODE in mRNA. Transfer RNA (tRNA)

25. Translation - 2

26. Translation - 3 • The GENETIC CODE is said to be TRANSLATEDinto a PROTEIN when the AMINO ACIDS brought bytRNApolymerize to form aPROTEIN. • The PRIMARY STRUCTURE of the PROTEIN (number, type and sequence of amino acids) is dictated by the PRIMARY STRUCTURE of the mRNA molecule (number, type and sequence of codons) which brought the GENETIC CODE to the ribosome and in turn by the GENE from which the mRNA was formed.

27. Overview of Protein Synthesis - 2 Transcription Translation 5' tRNA molecules (bind to large ribosome subunit) Next anticodon will be AAA First amino acid Next amino acid will be phenylalanine

28. The Genetic Code • Note that the genetic code is • a triplet code • redundant (only 20 amino acids but 64 codons- 3rd base of many codons can vary so a mutation here is not damaging)

29. Semi - Conservative DNA Replication • When DNA replicates prior to cell division each strand acts as a “template” for making one new strand. • Thus each new double helix consists of one “old” or parent strand and one “new” or daughter strand. • For this reason the process is called • SEMI - CONSERVATIVE DNA REPLICATION. • DNA REPLICATION begins when DNA uncoils. • Free DNA NUCLEOTIDES then base pair with nucleotides in each of the parent DNA strands using the enzyme DNA Polymerase. • These nucleotides then join together to form a new daughter strand that is complementary to the parent strand from which it was formed.

30. DNA Replication - 2 Step 1: Parent DNA strands separate.

31. DNA Replication - 3 Step 2: Each parent strand acts as a template for a new DNA strand growing antiparallel to the old strand in a 5 ’----> 3’ direction. 5’ 3’ Each new DNA strand grows in 5’------> 3’ direction Base pairing 5’ 3’

32. DNA Replication - 4 Two new identical DNA molecules are formed, each with one old strand and one new strand. 5’ Parent DNA strands 3’ 3’ 5’ New DNA strands New DNA molecule New DNA molecule H bonds between base pairs 3’ 5’ 3’ 5’

33. DNA Replication - Summary • Parent DNA molecule “unzips at Origin of Replication • “Replication Fork” New “leading” DNA strand grows continuously in a 5’--->3’ direction towards replication fork New “lagging” DNA strand grows in fragments in a 5’--->3’ direction away from replication fork Campbell & Reece, fig. 17.27

34. Gene (Point) Mutations • According to the ONE GENE ONE PROTEIN THEORY for each PROTEIN in the body there is aGENEwhich controls it. There is therefore a ONE -TO-ONE RELATIONSHIP between PROTEINS and GENES and between CODONS in a GENE andAMINO ACIDSin the PROTEIN controlled by the GENE. • A single GENE (POINT) MUTATION consists of a CHANGE in oneBASE within a CODON. This, in turn, will change theAMINO ACIDSEQUENCE in the PROTEIN controlled by the GENE. • A single BASE SUBSTITUTION in a gene will change ONE CODON only and may therefore affect only ONEAMINO ACIDin the protein.

35. Base Substitution Mutations Normal mRNA Base substitution at 3rd position of codon usually has no effect on protein If a STOP CODON results from a base substitution a NONSENSE MUTATION occurs forming a shortened polypeptide. A single BASE SUBSTITUTION in a gene will change ONE CODON only and may therefore affect only ONEAMINO ACIDin the protein.

36. Sickle Cell Gene: A Base Substitution Mutation Sickle cell Normal RBC HbS sickles when blood O2 is low (Beta chain) (Beta chain) Hydrophobic valine less soluble Abormal DNA codon for valine instead of glutamic acid Normal DNA codon for glutamic acid

37. Base Insertion or Deletion Mutations Normal reading “frame” Normal mRNA • BASE ADDITION or BASE DELETION MUTATIONS are “frame shift” mutations and will affect every codon after that point in the gene. • These mutations are therefore more serious since they may change every amino acid after that point in the protein Base addition - Reading “frame” shifts to left Base deletion - Reading “frame” shifts to right

38. Enzyme Deficiency Diseases (Inborn Errors of Metabolism) • Since almost all ENZYMES are PROTEINS, each ENZYME must be controlled by a GENE. • A GENE MUTATION in this case would result in the ABSENCE of the ENZYME, a condition called an ENZYME - DEFICIENCY DISEASE. • These inherited diseases were first described by Garrod in 1909 and called “INBORN ERRORS OF METABOLISM”. • Inborn Errors of Metabolism include • - PKU disease • - Galactosemia • - familial hypercholesterolemia • - von Gierke’s disease (and other glycogen storage diseases)

39. Somatic vs Germ Cell Mutations • Since DNA is faithfully copied during DNAREPLICATION,SOMATIC CELL MUTATIONS are passed on to all daughter cells. • However, only MUTATIONS in GERM CELLS (i.e.GAMETES) can be passed on to OFFSPRING.