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Forensic DNA Analysis
        Criminalist Harry Klann,
        DNA Technical Leader
        DNA Detail
        Los Angeles Police Department
        Scientific Investigation Division
        PowerPoint presentation by
        Criminalist Carl Matthies
Objectives of Forensic
    DNA Testing
    s   To link an individual to a crime
        scene/criminal act
    s   To exonerate suspects
    s   To identify victims of mass
        disasters
s   A Brief History
s   Contemporary Forensic DNA
    Testing
s   Casework Applications
s   Questions?
Early 1980s: Restriction Fragment
Length Polymorphism (RFLP)
                    s   Genetic variation in the distance
                        between restriction enzyme sites
                    s   Template DNA digested by
                        enzymes, electrophoresed,
                        detected via Southern blotting
Sir Alec Jeffreys
                    s   Power of discrimination in the
                        range of 106-108 for a six probe
                        analysis
Mechanisms
for RFLPs
Mid-1980s: The Colin Pitchfork Case
        s   Two young women raped and
            murdered in Narborough, England
        s   5,000 local men are asked to
            provide blood/saliva samples
        s   1st exoneration and conviction on
            forensic DNA evidence
The Catch:
s   RFLP testing requires a relatively
    large amount of HMW DNA
    (~50ng = thousands of cells)
s   Not ideal for forensic evidence, in
    which small, degraded samples
    are common
PCR To The Rescue!
                   s   Polymerase Chain Reaction =
                       molecular Xeroxing
                   s   Three temperature phases, carried
                       out in a Thermal Cycler, replicate
                       or “amplify” the desired DNA
Dr. Kary Mullis
Eccentric Genius       fragment(s)
PCR (cont’d)
s   First forensic application is the
    DQα locus, later multi-plexed with
    Polymarker™ loci using dot-blot
    detection method
s   Works with lower quantity (1-2ng),
    lower quality samples
s   Power of discrimination goes from
    102-106...not good enough for
    databasing
The Current Method of Choice:
Autosomal Short Tandem Repeats
        s   Non-coding, tetranucleotide
            sequences which vary greatly from
            person to person in the number of
            repeating units
        s   Requires <1ng of DNA to type
            13-15 STR loci
        s   Power of discrimination ranges
            from 1014-1023. World population is
            109 so bring on the database!
Applied Biosystems 310 Genetic Analyzer
The Process In a Nutshell
Amplified DNA samples are injected
into a capillary. Fluorescent tags on
the DNA fragments are excited by a
laser as they pass a window in the
capillary, the fluorescence is recorded
by a camera, and this signal is
converted into a “peak” by the
computer software.
STR data


X, Y,
   XY
STR data (cont’d)
STR data (cont’d)
                                                 STR TYPING SUMMARY SHEET
Date:                      DNA Analyst / Serial #:                                            DR #:

9/24/1999                  MATTHIES                               V9780                       00-00-00001
 Item #   AMEL   D3S1358     vWA       FGA     D8S1179   D21S11   D18S51   D5S818   D13S317   D7S820   D16S539   THO1   TPOX

          X, Y     17                                                                          8, 10
 25(S)                     15, 17 23, 26 14, 15           26      12, 15    10      9, 13              9, 10     8, 9   9, 10
          X, Y     17                                                                          8, 10
            X    15, 17                                  28,                                    11
 25(E)                     16, 18 19, 26         15               14, 16   8, 13      12               11, 12    7, 8    11
            X    15, 17                                  32.2                                   11
            X    15, 17                                  28,                                    11
VICTIM                     16, 18 19, 26         15               14, 16   8, 13      12               11, 12    7, 8    11
            X    15, 17                                  32.2                                   11
          X, Y     17                                                                          8, 10
SUSPECT                    15, 17 23, 26 14, 15           26      12, 15    10      9, 13              9, 10     8, 9   9, 10
          X, Y     17                                                                          8, 10



 “The DNA profile obtained from Item 25(S) matches the
 DNA profile of the suspect. The combination of genetic
 marker types exhibited by Item 25(S) and the suspect
 occurs in approximately one in one hundred quadrillion
 (1017) individuals…”
How are these astronomical figures derived?
The product rule: combined probability of a series of independent
events is determined by multiplying the probabilities of each event.
STR loci are inherited independently (unlinked)
Homozygous loci: p2 (same allele inherited from mother and father)
Heterozygous loci: 2pq (either allele could be inherited from either
parent)
p(17)2 x 2p(15)q(17) x 2p(23)q(26)….
(.223)2 x 2(.083)(.25) x 2(.14)(.02) = .000013, which is equivalent
to a probability of one in 76,000 using just 3 of the 13 loci!
STR Artifacts
-A (“minus A”): Incomplete addition of
nucleotide ‘A’ by DNA polymerase;
results in a peak that is one base pair
smaller than allele peak.
STR Artifacts

Stutter: Slippage of DNA polymerase;
results in a peak that is four base pairs
(one repeat unit) smaller than allele peak.
STR Artifacts

Pull-up: Incomplete filtration of spectral
overlap in fluorescent detection system.
Pull-up
DNA Mixtures




When more than one source of DNA is detected in a sample,
assignment of genotypes becomes more difficult.
Degraded/Trace DNA Samples




Larger alleles “drop-out” when template DNA is low in
quantity or quality, reducing certainty of genotypes.
The Combined DNA Index System
           (CoDIS)
         s   A database of DNA profiles from
             violent felons and crime scene
             samples
         s   Laws concerning who is eligible for
             the database vary from state to
             state
         s   Database currently contains about
             2,038,470 felons and 93,956 crime
             scene profiles (19,00 hits so far)
The Mystical Power of CoDIS

       s   Extremely powerful investigative
           tool, linking crimes, and pulling
           suspects out of thin air!
       s   Can prevent, as well as solve
           crimes!
The Dark Side of CoDIS
 (What the FBI doesn’t want you to know.)

         s   DNA mixtures and degraded DNA
             profiles have lead to spurious
             matches
         s   Stringent laws explicitly permit
             databasing innocent people
         s   Adding arrestees to database
             violates presumption of innocence
         s   However, the prosecution rate on
             case to offender matches is
             shockingly low! (~10%)
LAPD CoDIS Statistics
    s   177/142 Case-to-Offender
        matches
    s   100 Case-to-Case hits with 42 as
        yet unidentified suspects
    s   28 DA “rejects”
    s   9 Convictions; charges filed in 28
        more; 4 defendants plead guilty
    s   280 investigations aided…
“Specialized” PCR-based systems
            s   mtDNA
            s   Y-STRs
            s   SNPs
Mitochondrial DNA (mtDNA)
Mitochondrial DNA (mtDNA)
                         Pros
s   Single-cell sensitivity because each cell
    contains ~1000 mitochondria
s   Especially useful for shed hairs, burnt
    remains
s   Can be used to establish kinship directly
    because entire complement of mtDNA is
    maternally inherited
Mitochondrial DNA (mtDNA)
                         Cons
s   Single-cell sensitivity because each cell
    contains ~1000 mitochondria = very high
    contamination risk!
s   Heteroplasmy - more than one mtDNA type
    manifesting in different tissues in the same
    individual
s   Lower power of discrimination - maternal
    relatives all share the same mtDNA
Y-STRs
                     Problem:
s   ~99% of violent crimes are committed by
    men
s   DNA Mixtures of male suspect and female
    victim can pose an analytical challenge,
    especially when the female contribution is
    much greater than the male = preferential
    amplification
Y-STRs
                      Solution:
s   Test for markers found only on the Y-
    chromosome. Only male DNA is amplified!
Y-STRs
                   “Khan” Argument
s   Lower power of discrimination - paternal
    relatives all share the same Y-STR
    haplotype (“Wicked Uncle Ernie” Defense)
s   10% of Central Asian males share the same
    Y-STR haplotype, thought to belong to
    Genghis Khan
Single Nucleotide Polymorphisms (SNPs)

 s   Point mutations (base substitutions) found in
     1% or more of the population
 s   1.8 million identified in human genome
 s   Detected on micro-array plates with
     fluorescent tags (all or nothing response)
SNPs (cont’d)


s   ~50 SNPs provides same power of
    discrimination as 13 STR loci
s   Certain SNPs used as predictors of
    ancestry/ethnicity by a private sector lab
    (DNA Witness)
Flawed logic in the use of SNPs for predicting ancestry

 Scenario 1:
  SNP profile inconsistent with subject’s
   reported ancestry ¿ subject’s family history is
   inaccurate ¿ results are indisputable
 Scenario 2:
  SNP profile inconsistent with subject’s
   physical appearance ¿ ad hoc human
   migration explanation ¿ results are
   indisputable
Other SNP Flaws
s   Privacy issues - unlike STRs, SNPs can be
    correlated with susceptibility/resistance to
    diseases
s   Requires a relatively large quantity of DNA for
    robust assay

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Forensic DNA Analysis Techniques and Applications

  • 1. Forensic DNA Analysis Criminalist Harry Klann, DNA Technical Leader DNA Detail Los Angeles Police Department Scientific Investigation Division PowerPoint presentation by Criminalist Carl Matthies
  • 2. Objectives of Forensic DNA Testing s To link an individual to a crime scene/criminal act s To exonerate suspects s To identify victims of mass disasters
  • 3. s A Brief History s Contemporary Forensic DNA Testing s Casework Applications s Questions?
  • 4. Early 1980s: Restriction Fragment Length Polymorphism (RFLP) s Genetic variation in the distance between restriction enzyme sites s Template DNA digested by enzymes, electrophoresed, detected via Southern blotting Sir Alec Jeffreys s Power of discrimination in the range of 106-108 for a six probe analysis
  • 6. Mid-1980s: The Colin Pitchfork Case s Two young women raped and murdered in Narborough, England s 5,000 local men are asked to provide blood/saliva samples s 1st exoneration and conviction on forensic DNA evidence
  • 7. The Catch: s RFLP testing requires a relatively large amount of HMW DNA (~50ng = thousands of cells) s Not ideal for forensic evidence, in which small, degraded samples are common
  • 8. PCR To The Rescue! s Polymerase Chain Reaction = molecular Xeroxing s Three temperature phases, carried out in a Thermal Cycler, replicate or “amplify” the desired DNA Dr. Kary Mullis Eccentric Genius fragment(s)
  • 9.
  • 10. PCR (cont’d) s First forensic application is the DQα locus, later multi-plexed with Polymarker™ loci using dot-blot detection method s Works with lower quantity (1-2ng), lower quality samples s Power of discrimination goes from 102-106...not good enough for databasing
  • 11. The Current Method of Choice: Autosomal Short Tandem Repeats s Non-coding, tetranucleotide sequences which vary greatly from person to person in the number of repeating units s Requires <1ng of DNA to type 13-15 STR loci s Power of discrimination ranges from 1014-1023. World population is 109 so bring on the database!
  • 12. Applied Biosystems 310 Genetic Analyzer
  • 13. The Process In a Nutshell Amplified DNA samples are injected into a capillary. Fluorescent tags on the DNA fragments are excited by a laser as they pass a window in the capillary, the fluorescence is recorded by a camera, and this signal is converted into a “peak” by the computer software.
  • 16. STR data (cont’d) STR TYPING SUMMARY SHEET Date: DNA Analyst / Serial #: DR #: 9/24/1999 MATTHIES V9780 00-00-00001 Item # AMEL D3S1358 vWA FGA D8S1179 D21S11 D18S51 D5S818 D13S317 D7S820 D16S539 THO1 TPOX X, Y 17 8, 10 25(S) 15, 17 23, 26 14, 15 26 12, 15 10 9, 13 9, 10 8, 9 9, 10 X, Y 17 8, 10 X 15, 17 28, 11 25(E) 16, 18 19, 26 15 14, 16 8, 13 12 11, 12 7, 8 11 X 15, 17 32.2 11 X 15, 17 28, 11 VICTIM 16, 18 19, 26 15 14, 16 8, 13 12 11, 12 7, 8 11 X 15, 17 32.2 11 X, Y 17 8, 10 SUSPECT 15, 17 23, 26 14, 15 26 12, 15 10 9, 13 9, 10 8, 9 9, 10 X, Y 17 8, 10 “The DNA profile obtained from Item 25(S) matches the DNA profile of the suspect. The combination of genetic marker types exhibited by Item 25(S) and the suspect occurs in approximately one in one hundred quadrillion (1017) individuals…”
  • 17. How are these astronomical figures derived? The product rule: combined probability of a series of independent events is determined by multiplying the probabilities of each event. STR loci are inherited independently (unlinked) Homozygous loci: p2 (same allele inherited from mother and father) Heterozygous loci: 2pq (either allele could be inherited from either parent) p(17)2 x 2p(15)q(17) x 2p(23)q(26)…. (.223)2 x 2(.083)(.25) x 2(.14)(.02) = .000013, which is equivalent to a probability of one in 76,000 using just 3 of the 13 loci!
  • 18. STR Artifacts -A (“minus A”): Incomplete addition of nucleotide ‘A’ by DNA polymerase; results in a peak that is one base pair smaller than allele peak.
  • 19. STR Artifacts Stutter: Slippage of DNA polymerase; results in a peak that is four base pairs (one repeat unit) smaller than allele peak.
  • 20. STR Artifacts Pull-up: Incomplete filtration of spectral overlap in fluorescent detection system.
  • 22. DNA Mixtures When more than one source of DNA is detected in a sample, assignment of genotypes becomes more difficult.
  • 23. Degraded/Trace DNA Samples Larger alleles “drop-out” when template DNA is low in quantity or quality, reducing certainty of genotypes.
  • 24. The Combined DNA Index System (CoDIS) s A database of DNA profiles from violent felons and crime scene samples s Laws concerning who is eligible for the database vary from state to state s Database currently contains about 2,038,470 felons and 93,956 crime scene profiles (19,00 hits so far)
  • 25. The Mystical Power of CoDIS s Extremely powerful investigative tool, linking crimes, and pulling suspects out of thin air! s Can prevent, as well as solve crimes!
  • 26. The Dark Side of CoDIS (What the FBI doesn’t want you to know.) s DNA mixtures and degraded DNA profiles have lead to spurious matches s Stringent laws explicitly permit databasing innocent people s Adding arrestees to database violates presumption of innocence s However, the prosecution rate on case to offender matches is shockingly low! (~10%)
  • 27. LAPD CoDIS Statistics s 177/142 Case-to-Offender matches s 100 Case-to-Case hits with 42 as yet unidentified suspects s 28 DA “rejects” s 9 Convictions; charges filed in 28 more; 4 defendants plead guilty s 280 investigations aided…
  • 28. “Specialized” PCR-based systems s mtDNA s Y-STRs s SNPs
  • 30. Mitochondrial DNA (mtDNA) Pros s Single-cell sensitivity because each cell contains ~1000 mitochondria s Especially useful for shed hairs, burnt remains s Can be used to establish kinship directly because entire complement of mtDNA is maternally inherited
  • 31. Mitochondrial DNA (mtDNA) Cons s Single-cell sensitivity because each cell contains ~1000 mitochondria = very high contamination risk! s Heteroplasmy - more than one mtDNA type manifesting in different tissues in the same individual s Lower power of discrimination - maternal relatives all share the same mtDNA
  • 32. Y-STRs Problem: s ~99% of violent crimes are committed by men s DNA Mixtures of male suspect and female victim can pose an analytical challenge, especially when the female contribution is much greater than the male = preferential amplification
  • 33. Y-STRs Solution: s Test for markers found only on the Y- chromosome. Only male DNA is amplified!
  • 34.
  • 35. Y-STRs “Khan” Argument s Lower power of discrimination - paternal relatives all share the same Y-STR haplotype (“Wicked Uncle Ernie” Defense) s 10% of Central Asian males share the same Y-STR haplotype, thought to belong to Genghis Khan
  • 36. Single Nucleotide Polymorphisms (SNPs) s Point mutations (base substitutions) found in 1% or more of the population s 1.8 million identified in human genome s Detected on micro-array plates with fluorescent tags (all or nothing response)
  • 37. SNPs (cont’d) s ~50 SNPs provides same power of discrimination as 13 STR loci s Certain SNPs used as predictors of ancestry/ethnicity by a private sector lab (DNA Witness)
  • 38. Flawed logic in the use of SNPs for predicting ancestry Scenario 1: SNP profile inconsistent with subject’s reported ancestry ¿ subject’s family history is inaccurate ¿ results are indisputable Scenario 2: SNP profile inconsistent with subject’s physical appearance ¿ ad hoc human migration explanation ¿ results are indisputable
  • 39. Other SNP Flaws s Privacy issues - unlike STRs, SNPs can be correlated with susceptibility/resistance to diseases s Requires a relatively large quantity of DNA for robust assay

Hinweis der Redaktion

  1. Mass disasters can be either manmade (9/11 act of terrorism) or natural (2005 Indian Ocean Tsunami, 295,000 dead)
  2. “Please just call me Alec.”
  3. “ The Blooding” by Joseph Wambaugh, retired LAPD Sergeant
  4. DNA mixtures can be tricky; requiring close examination of the electronic data, the questioned profile, and the offender “match” profiles. For example, an unknown mixture profile with three alleles at the D21S11 locus, ex. (28, 30, 31) would “hit” on (28, 28), (28, 30), (28, 31), (30, 30), (30, 31), and (31, 31). A total of 6 genotypes. If we designate an obligate or required allele (+), (28, 30+, 31)* would now hit only on the following genotypes: (28, 30), (30, 30), and (30, 31). We have reduced the number of hits at the D21S11 locus by half. Assigning obligate alleles at as many loci as possible can reduce the number of spurious hits to the offender database. * In this example, which could be a vaginal swab taken from the victim of a sexual assault, the victim was determined to be a (28, 31) at D21S11. Therefore, the 30 allele is foreign to the victim and presumed to be from the suspect.
  5. 177 cases matched to 142 offenders California State DNA Index System (SDIS): 304,817 offender STR profiles 9,633 forensic STR profiles
  6. Scenario 2: LAPD Detective Tom M., SNPs 62% European, but appears SE Asian/Indian.