overview of research methods in dentistry robert weyant, dmd drph department of dental public health...

Overview of Research Methods in Dentistry

Robert Weyant, DMD DrPHDepartment of Dental Public Health and Information Management

University of Pittsburgh

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What is “Causation”

• Koch-Henle postulates • Bradford-Hill 'criteria' • inductionist, refutationist, or hypothetico-

deductivist view• Provides the basis for “intervention”

"Causality. There is no escape from it, we are forever slaves to it. Our only hope, our only peace is to understand it, to

understand the why”Larry, .; Andy Wachowski, . The Matrix: Reloaded.

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Hills Criteria of Causation• Austin Bradford Hill (1897-1991),

a British medical statistician as a way of determining the causal link between a specific factor (e.g., cigarette smoking) and a disease (such as emphysema or lung cancer).

• Hill's Criteria form the basis of modern epidemiological research, which attempts to establish scientifically valid causal connections (disease – and its cause)

• Temporal Relationship• Strength• Dose-Response

Relationship• Consistency• Plausibility• Consideration of Alternate

Explanations• Experiment• Specificity• Coherence

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Systems

• Deterministic Systems • Events are part of an

unbroken chain of prior occurrences.

• Outcomes occur predictably

• Newtonian Physics

• Stochastic Systems • Outcomes are

computationally and practically unpredictable.

• Present state does not fully determine the next state

• Biology and medicine are stochastic

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Statistical Causality• Observational studies (like counting cancer cases among smokers and among

non-smokers and then comparing the two) can give hints, but can never establish cause and effect.

• Hypothesis generation.• The gold standard for causation here is the randomized experiment:

• One limitation of experiment is they do a good job of testing for the presence of some causal effect they do less well at estimating the size of that effect in a population of interest.

• Subject selection may lack generalizability.• .

Exp

Med

Outcome

Research Designs

In clinical research

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Essentials of Research Design

• Basic research• Clinical research (often experimental)

• Epidemiological research (often observational, know denominator)

• Health services research

limited to human research (in vivo)

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What are our research

(and clinical) concerns?• Exposure

• Good or bad: Chemical, biological, psychological, educational, etc.

• Outcome• Good or bad: disease, cure, improved attitude,

longer life, etc.

• We generally know one and want to measure the other

• Concerns are that we measure both accurately and understand what population is represented.

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Classification Schemes• Descriptive vs. Analytical• Experimental vs. Observational• Time Referenced

• Prospective vs. Cross-sectional vs. Retrospective

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Describe or Analyze?

• Descriptive• simply describe what was seen (common in

surveys). Prevalence of various conditions. • PREVALENCE: the proportion of the population who

exhibit the condition of interest.

• Analytic• attempt to determine the associations between

disease and possible risk factors/determinates and to quantify risk. (common for experimental designs and search for causality)

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Experiment or Observe?

• Experimentation is defined by the degree of control or manipulation the investigator has over the study conditions.

• In a non-experimental (observational) design the investigator has less control over the study conditions.

• The consequences of study design are in the limitations put upon the interpretation of the results of the study.

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Time

Cross Sectional

Time

Retrospective

Case control

? $Prospective

All experimental and cohort (obs)

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Classification according to CONTROL / INTERVENTION

• Experimental Designs (Classic Design = RCT)

• Prospective• Investigator alters the conditions understudy• There is a true control group• Randomization MUST occur

• Observational• May be prospective/retrospective/cross-sectional• No control• No intervention

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Issues of concern

1. Population

2. Control group

3. Sample size

4. Placebo

5. Control of Operational Procedures

6. Validity and Reliability of Measures

7. Duration

8. Statistical Analysis

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1. Population (Relevance)

• When you read a study you must ask: • is the population representative of

something I care about? • Is it appropriate to answer the question.

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How do people get into a “study”?

• They volunteer• Often they are in the right place at the

right time• They have the right disease (severity) or

exposure.• Often “clinic” based studies are very

poorly generalized to larger populations.

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Why people don’t get into a study

• Too sick or not sick enough• Wrong gender, race, etc….• Don’t live in the right place.• Don’t know about the study.

Population of interest(in community)

Barriers

Lack of knowledge

Referral Issues

Fear

Transportation

Present for study

Eligible

Barriers

Wrong disease severity

Demographic issues

Barriers

Fear

Transportation

Not willing to be “randomized”

Complete study and can be found for follow up

Generalizability of Results

Barriers

Not adhere to protocol

Lost to follow up (move, die)

Where do research “subjects” come from?

Consent/Enroll

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Is the study relevant and valid?

• External validity• Do the study subjects represent a definable

population of interest - i.e., “your patients”?• Hence, is it relevant

• Internal validity• Is the study well designed and analyzed?• Hence, is it valid

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2. Sample Size (did you look at enough people…)

• There must be enough people in the study to ensure that the conclusions are valid. The likelihood that a finding will be spurious or incorrect decreases as you increase the number of individuals in the study.

• POWER: the ability of a test to detect a significant difference when one exists. Be particularly attentive to negative studies.

• Function of effect size, variance, sample size

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3. Control Group ?(it worked!……compared to what?)

• If we are to conclude that an intervention has an effect, then we must be sure that the group with and without the intervention were similar before the study began/and remained so except for the intervention.

• If not, bias can result in spurious conclusions.

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4. Placebo ?(I feel much better...what was that?)

• Placebo is a material, formulation, intervention that is similar to the test product, but without the active ingredient.

• There is a well documented placebo effect in many situations.• Up to 70% in some studies.

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5. Control of operational procedures (What exactly did you do, doctor?)

• When reading a study for your own use, it is important that the authors explain precisely what they did. This allows the reader to generalize to his/her own situation and helps to assess relevance

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6. Reliability of measures (That was great…now do it again?)

• One of the most important areas in any study: did the effect occur and how do we know. Someone measured it. We must be able to determine that the investigator(s) measured it accurately, repeatable.

• INTRA-RATER reliability (same cases over time)• INTER-RATER reliability (comparison of same cases

among raters)• Instrumentation

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7. Duration of study(over so fast?)

• Did the trial run long enough to measure the desired effect.

• Caries trials 2-3 years• Calculus-preventing agents 90 days• Orthodontic outcomes (20 years?)• Implants (5 years)

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8. Statistical Analysis(So, did I find anything “significant?”)

• Where they appropriate to the design, quality of data, intent of investigators.

• Statistical analysis is based on type of data (nominal, ordinal, ratio).

• Type of question being asked• Summarize• Difference between groups• Effect size or risk

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Threats to Validity of a Study(Nice result, but what about…)

• Bias: Any systematic error in a study which results in an incorrect estimate of the association between disease and exposure.

• Confounding: results when there is a mixing of the effect of the exposure and disease with a “third factor”

• Chance: The exposure:disease relationship is spurious as the result of random variation in sampling.

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Types of Bias

• Selection• Non-representative sample• Non-comparable case/control groups• Loss to follow-up• Differential survival

• Observation (Misclassification error)• Disease Classification• Exposure Classification• Instrumentation

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Confounding

• Definition: the bias in the (crude) disease-exposure estimate that can result when the exposure-disease relationship is mixed up with the effect of “extraneous variables”

• Confounding affects our understanding of the “true” disease-exposure relationship

• The determination is “data-based”• Two methods

• Stratification• mulitvariate analysis

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Chance

• That’s what we have statistics for - to quantify the chance.

• Type 1 (alpha) error (p-value).

Research Designs

no

Observational studies

yes

Experimental studies

Is there to be a

control group

no

Do we know disease status of patients before study

Will observations bemade at more than onetime

yesCohort study

yesCase-control study

Cross sectional studyno

Alter the conditionsunder study

yes True experiment

no Quasi - Experiment

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Observational Designs

Cross SectionalCase Control (retrospective)

Cohort (prospective)

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Cross Sectional Study

• Measure, Classify, Compare• Used for questionnaires, surveys,

prevalence estimates, to generate hypotheses.

• Everything occurs “at once”.

Cross Sectional Design1. Select Pop of interest

Population of Interest

2. Select Sample

Study Sample

3. Assess population for both disease (outcome) status

Disease Positive

Disease Negative

RF +

RF +

RF -

RF -

and risk factor (exposure) status

Analyze using correlational statistics but causation not “provable” due to lack of temporal association

Cross-Sectional DesignAdvantage:

1. Quick and Low Cost

2. Evaluate a large number of variables

3. Enroll a large number of Subjects

Disadvantage:

1. Subject selection may reflect selection bias (volunteers, hospital patients)

2. Is difficult to identify cause and effect relationship.

Common Uses:• Questionnaires and Surveys• Prevalence studies• Hypothesis Development

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Case Control

• Select cases and controls• Retrospective assessment of risk factors• Quantify exposure. Since no

denominator, only relative rates.

Case-Control Design

1. Select group of subjects WITH disease/outcome of interest = CASES

Cases

2. Select group of subjects WITHOUT disease/outcome = CONTROLS

Controls

RF +

RF +

RF -

RF -

3. Measure (retrospectively) risk factors of interest.

4. Analyze using strength of association measures.

Selection of controls crucial

Case selection also must be carefully considered

Common Use:

Rare Disease (e.g., birth defects)

Long Latency (e.g., cancer)

Case-Control DesignAdvantages

1. not dependent on natural frequency of disease (thus used to study rare diseases)

2. well suited to study diseases with long latency

3. requires comparatively few cases (2:1 or 3:1 matching)

4. not dependent on previously established cohort

5. allows study of multiple potential causes of disease

6. relatively low cost and quick

7. ethical: disease has already occurred

Disadvantages

1. case selection may be problematic

2. controls may not be representative of same population as cases in terms of disease risk or confounders

3. investigators may be biased when know of disease status of subjects

4. subjects may bias answers (recall) due to disease status

5. factors which are used to match are removed from analysis

6. incidence, prevalence, RR and AR can't be calculated since no "population at risk" denominator is available

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Cohort Design

• Select two or more groups (cohorts) that are free of disease but differ on their exposure status.• May start with one heterogeneous cohort.

• Cohorts have a “denominator” which allows the calculation of true rates.

• Useful when “exposure” varies over time.

Cohort Study Design1. Select Population of interest

Population of Interest

2. Recruit sample WITHOUT disease(s) of interest and measure risk factors

Disease Free Study Sample

(baseline exam)

Prospective, Observational Design.

Uses:

• Determining/quantifying risk factors• Developing new etiological theory•Establishing causality

Visit 2

3. Recall cohort periodically and remeasure risk factors and disease status

Visit 3 Visit n

Time

Cohort DesignAdvantages

1. allows risk to be expressed as incidence

2. certain biases are reduced:

exposure status

disease status

3. subject characteristics can be related to more than one outcome

Disadvantages

1. inefficient for study of rare disease

2. assessment of relationships limited to those defined at beginning of study

3. selection bias not controlled

4. loss to follow-up common

5. subjects may change in regards to characteristics (i.e. exposure status)

6. bias may be present if the characteristic studied influences surveillance and if surveillance influences detection of outcome (Berkson's fallacy)

7. expensive and time consuming

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Experimental Designs

Clinical Trials (RCTs)

Field Trials

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Clinical Trials• Prospective controlled experiment of human

subjects to assess intervention for a specific disease.

• Asks an important research question• Clinical event or outcome• Done in clinical or medical setting• Evaluates one or more interventions compared

with “standard treatment”• Informed consent and DSMB required

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Phases of Clinical Trials

• Phase I: dose finding• Phase II: efficacy at fixed dose• Phase III: comparing treatment (RCT)• Phase IV: late/uncommon effects

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Uses of Clinical Trails (experimental studies)

• Test new drug therapy • Test new surgical interventions• Test educational/programatic

interventions

Randomized Clinical Trial Design

1. Recruit individuals WITH disease.

Study Sample

with disease

Randomization is essential, and along with strict control of experimental conditions allows for minimal bias

Excellent internal validity (but possibly low external validity)

2. Randomize into treatment arms

Standard Treatment

New Treatment

Randomization

Outcomes

Outcomes

3. Follow up to assess outcomes

Ethical only to the degree that differences in treatment are unknown at time of study initiation (equipoise). Requires DSMB.

Experimental DesignAdvantages

1. investigator directly controls assignment to study groups

2. investigator directly controls exposure to agent.

3. random assignment measures can control extraneous factors.

4. blinding of evaluators may be possible

Disadvantages:

1. not immune to problems encountered with other designs: (non-compliance, incomplete follow-up, biased observation)

2. may have low external validity

3. may not be feasible for studies of disease etiology (ethical considerations, rare disease)

4. may not be feasible for effective disease prevention exists. (can't withhold treatment)

5. Can be very expensive

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Efficacy vs. Effectiveness

• Efficacy is the potential to provide a clinical benefit.

• Measured in CTs

• Effectiveness is the benefit provided in routine “real world” use.

• Measured in surveillance systems (registries), after market incident reports, etc.

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Hierarchy of Research Designs

• Experimental designs• Cohort studies• Case-control designs• Human trial without controls• Cross-sectional designs• Descriptive studies• Case reports• Personal opinion

Based on control of bias and confounding and ability to make causal arguments

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RCT’s Strengths

• Minimally biased design• Randomization• Control of extraneous variables

• Prospective (causality established)• Design issues determined prior to initiation of

study.

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Problems with (Dental) RCTs• Difficult to randomize• Ethical Concerns

• Principle of Equipoise involves the ethical treatment of human subjects in experimental conditions. A subject should only be submitted to a randomized, controlled design if there is substantial uncertainty about which of the treatments would benefit the subject most.

• RCTs should not be done when patient preference can be elicited (ortho vs. surgical tx)

• Blinding issues (Hawthorne effect)• Expensive (and often lack sponsor)

What are the current “Issues” in Dental clinical research?

• Diagnosis• Treatment approach• Materials• Long term issues

• Harm

• Health Services Research

• Cost Effectiveness

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Negative Study

• No association• Sloppy design (poor methods or

analysis)• Bias• Chance

• Statistics measures “chance” (expressed as p-value)

Systematic Reviews

Putting it all together

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Scientific Truth relies on• the weight of evidence over many studies that creates

confidence in results. • If its not published….it didn’t happen.

• Journalistic Reviews…the “old way”• Remember the essays you used to write as a student? You would

browse through the indexes of books and journals until you came across a paragraph that looked relevant, and copied it out. If anything you found did not fit in with the theory you were proposing, you left it out.

• Or the way its done by senior academics. Take a simmering topic, extract the juice of an argument, add the essence of one filing cabinet, sprinkle liberally with your own publications and sift out the work of noted detractors or adversaries…or

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Systematic Reviews…the new way

• In contrast to the old way, systematic reviews use explicit and rigorous methods to identify, critically appraise, and synthesize relevant studies.

• Qualitative: when the results of studies are not statistically combined.

• Quantitative or Meta-analysis: systematic review that uses statistical methods to combine the results of two or more studies

Maturation of DentistryMaturation of Dentistry

Age of Empiricism: Dental practice based on observation and experience in ignorance of scientific findings

Age of EvidenceDental practice based on high quality evidence of effectiveness

All knowledge maintained personally

Textbooks and Journals

Internet

Apprentice Model of Education

Scientific Literature and Knowledge Synthesis-based Education

Absence of Research

RCTsSystematic Reviews and Meta Analysis

Evolution of the Dental Knowledge Base

• store of specialized information - diseases - treatment methods - treatment outcomes • basis of professional decision-making • has evolved over time with respect to:

- creation- synthesis- dissemination

Bader JEBDP 2004

What is a Systematic Review• A "systematic review” comprehensively locates,

evaluates and synthesizes all the available literature on a given topic using a strict scientific design which must itself be reported in the review.

• Aim of SR is:• Systematic (e.g. in its identification of literature)• Explicit (e.g. in its statement of objectives, materials and

methods)• Reproducible (e.g. in its methodology and conclusions)

• Goal: To efficiently integrate valid information and provide a basis for rational decision making.

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Features of a Systematic Review

• Explicit criteria (reproducible)• Efficient

• As it is impractical for even an expert to read all the literature published in his field. SR are a succinct but robust form for practitioners who need to keep up to date?

• Well focused (PICO)• Thorough (unpublished information may be included)

• Provides a context for studies and creates a sense of the “weight of evidence”

• Secondary data analysis

Why Systematic Reviews• Annually 3 million articles are published in

biomedical journals and biomedicine mass doubling time is less than 20 months.

• You would need to read a dozen or more articles per day (365 days/yr.) to stay up to date.

• Not all articles are valid or useful for patient care.• SR provide a summary and context of the current

state of knowledge (that is lacking if you only read a few articles in an area).

Quality of Evidence Pyramid

Meta-Analysis

Systematic Review

Randomized Controlled Trial

Cohort studies

Case Control studies

Case Series/Case Reports

Basic Research and Animal research

}Guidelines

Questions come in two varieties:

• BACKGROUND QUESTIONS• Textbooks/Basic Sci Faculty

• FOREGROUND QUESTIONS• Clinical Faculty• Journal articles • Guidelines

BackgroundForeground

Dental School Professional Practice

Background Questions

• Are general questions about conditions, illnesses, syndromes and patterns of disease, and pathophysiology.

• "What is the typical clinical  presentation of primary oral herpes?” or

• “Which teeth are most commonly affected during ECC?”

• Novices asks this type of question in a  particular knowledge area, in order to gain a general understanding of clinical issues.

• Best resources include textbooks and faculty.

Foreground Questions• Foreground questions are about issues of patient

care and clinical decision-making. • Best resources:

• guidelines, • systematic reviews

Remember: Generally, its not what you don’t know that causes problems - its what you “know” that just ain't so….

Steps in Developing Systematic Reveiws

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Step 1: Identify an area of Uncertainty

• Diagnosis• How well does DIAGNODENT diagnosis interproximal caries?

• Therapy• Should asymptomatic impacted third molars be extracted?

• Prognosis• How long will a implant last when used to replace a single

anterior tooth lost due to trauma? Is it different if the tooth loss is due to perio?

• Harm or Causality• Do posterior inlays result in greater risk of tooth sensitivity

compared with other posterior restorations?

Step 2: Frame it as an Answerable Questions (PICO Format)

• P patients or populations• I interventions• C comparison group(s) or "gold standard"• O outcome(s) of interest

P.I.C.O.Patient or Problem

Intervention (a cause, prognostic factor, treatment etc.

Comparison Intervention (if necessary)

Outcomes

Tips for Building Questions

Starting with your patient, ask “How would I describe a group of patients similar to mine?”

Balance precision with brevity.

Ask “Which main intervention am I considering”

Be specific

Ask “What is the main alternative to compare with the intervention?”

Be specific

Ask “What can I hope to accomplish?”, or “What could this exposure really affect?”

Be specific

Example

In young adults will asymptomatic impacted third molars, cause ortho relapse or lead to problems better dealt with prophylactically

Surgical extraction Watchful waiting reduction of ortho relapse, prevention of oral infections, reduction in surgical complications at an older age.

Step 3: Search for the Evidence

• Philosophy: Find all literature that is relevant and valid

• Eliminate studies with poor design • Reduce potential for bias

• Effect size (design effects)• Publication (no negative studies)• Author (COI)• Poor search strategies

Step 3: Search for the Evidence

• Establish inclusion and exclusion criteria• Type of study (RCTs, Cohort, Case-Control,

Cross sectional)• Type of exposure and outcomes

• Case Definition• Exposure Definition• Are Outcomes Important (to whom?)

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Step 3: Search for the Evidence

• Develop Search Strategy• Electronic Databases

• MEDLINE, EMBASE, Cochrane Library, etc.• Search Filter (are they tested and sensitive/specific)

• Hand searching• Unpublished studies

• Gray literature (conference proceedings, disssertations)

• Reference lists• Personal communication

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Step 4: Extract Data

• Apply Inclusion and exclusion criteria• Two stage review (title/abstract; full article)• Two reviewers• Rules for resolving disagreements • Use predetermined forms• Log reason for exclusion

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Step 5: Analyze and Present Results

• Evidence Table• Research design• Subjects• Methods• Results

• Qualitative Summary• Quantitative Summary

• Heterogeneity• Meta-analysis• Sensitivity analysis

• Methodological Quality• allocation concealment • blinding • statistical analysis• funding/sponsorship• population (specificity)• intervention (specificity)• outcomes (specificity)

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Step 6: Interpret and Review Results

• Have all the main outcomes been considered• Have data been presented about absolute

change as a result of the intervention• Have any factors that may limit application been

considered• Are the results consistent• Don’t confuse “no evidence of an effect” with

“evidence of no effect”

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Forest Plots

A quick look at meta-analysis

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there’s a label to tellyou what the comparisonis and what the outcomeof interest is

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At the bottom there’sa horizontal line. This is the scale measuringthe treatment effect.Here the outcome is deathand towards the left thescale is less than one,meaning the treatmenthas made death lesslikely.

Take care to read whatthe labels say – things tothe left do not always meanthe treatment is better thanthe control.

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The vertical line in themiddle is where thetreatment and control have the same effect – there is no differencebetween the two

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For each study there is an id

The data foreach trial are here, divided into the experimental and control groups

This is the % weightgiven to thisstudy in the pooled analysis

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•Each study is given a blob, placed where the data measure the effect.•The size of the blob is proportional to the % weight •The horizontal line is called a confidence interval and is a measure of how we think the result of this study might vary with the play of chance. •The wider the horizontal line is, the less confident we are of the observed effect.

The label above the graph tells you what statistic has been used

The data shown in the graph are also given numerically

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The pooled analysis is given a diamond shapewhere the widest bit in the middle is located at the calculated best guess (point estimate), and the horizontal width is the confidence interval

Definition of a 95% confidence interval: If a trial was repeated 100 times, then 95 out of those 100 times, the best guess (point estimate) would lie within this interval.

At the end of the day….

What do we really want to know?

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Can we believe it ?

• bias free search & inclusion criteria?• appraisal of methodology of primary

studies?• consistent results from all primary

studies?• if not, are the differences sensibly explained?

• are the conclusions supported by the data?

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If we believe it — does it apply to our patient?

• Is our patient (or population) so different from those in the primary studies that the results may not apply?

• consider differences in:• time — many things change.• culture — both treatments and values of

outcomes can be different• stage of illness or prevalence can effect

results.

We believe it ! But….does it matter?

• Is the benefit worthwhile to our patient?• Ask the patient about cultural values.• Think about Relative Risk Reduction vs.

Absolute Risk to our patient.• Potential benefit is the Absolute risk

avoided in our patient = Absolute Risk Reduction (ARR)!

Is it a systematic review? does it:

• define a four part (answerable) clinical question?

• combine Randomized Controlled Trials (RCT’s)?

• describe PRE-DEFINED search methods?• PRE-DEFINED inclusion criteria?• PRE-DEFINED methodological exclusion

criteria?

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

Population

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

Population

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

Intervention

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

Intervention

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

Comparison

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

Comparison

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

Outcome

PICO Practice

“What is the effectiveness of semiannual fluoride varnish compared to semiannual fluoride gel in preventing dental caries in permanent teeth among caries-active adults?”

Egger at al., 2001

Step 1: Key Clinical Question

Outcome

PICO Practice

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Source of Secondary Information

• Systematic Reviews• E.g., Cochrane Collaboration

• Guidelines• E.g., National Guidelines Clearinghouse

THE COCHRANECOLLABORATION

Cochrane Collaboration

• An international organisation that aims to help people make well-informed decisions about healthcare by preparing, maintaining and promoting the accessibility of systematic reviews of the effects of health care interventions.

Cochrane Centres

South African

Australasian

Chinese

Brazilian

Nordic

German

San Antonio

ItalianIberoamerican

French

Dutch

UK

Canadian

New England

San Francisco

Cochran Library

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Evaluation of Diagnostic Tests

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Topics1. How do we “know” something.

• Scientific Reasoning

2. What are the elements and structure of scientific thinking.

• Facts, Hypotheses, Theories, Paradigms

3. Research Designs and Control of Bias4. Clinical Epidemiology

• Sensitivity, Specificity, Predictive Value

5. Measurement in Dentistry6. The Research Enterprise

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Topics1. How do we “know” something.

• Scientific Reasoning

2. What are the elements and structure of scientific thinking.

• Facts, Hypotheses, Theories, Paradigms

3. Research Designs and Control of Bias4. Clinical Epidemiology

• Sensitivity, Specificity, Predictive Value

5. Measurement in Dentistry6. The Research Enterprise

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Diagnostic Tests

• Purpose: to increase our certainty about the cause of a patients illness

• Common Types:• Physical and history findings• Laboratory test• Radiography• “Other” technological findings (pulp tester,

etc.)

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Examples of Diagnostic Tests in Dentistry• Caries

• visual, radiography, DIFOTI• Pulpal necrosis

• Electrical, thermal • Soft tissue lesions

• Biopsy, dye• Periodontitis

• Future attachment loss, PSR• Malocclusion

• Index, study models, ceph

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Reduction of Diagnostic Information• Scales• Indexes, • Cut Points• Basic Decision: Treat or No Treatment

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Outcomes in Orthodontics

• Malocclusion is not a disease• Outcomes based on clinician

assumptions of patients needs/desires• Many dimensions need to be measured

• Overjet, overbite, cross bite, etc…

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Measurement Issues in Orthodontics

• Index - assign numerical rating• Diagnostic (Angle)• Epidemiological Index (Summer’s)• Treatment need (HLD, Salzman, IOTN)• Treatment Outcome (PAR)

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Valid and Reliable

Reliable but NOT valid

NOT reliable or valid

Reliable and valid

Can’t be valid unless reliable

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What is validity in Ortho Index

• Measures dimensions of occlusion that are considered clinically important. These could based upon:• Expert opinion• Clinical consequences (disease) or

change• Patient values and desires

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How to assess reliability

• Intra-rater• Have same person rate the “case” more than once.

• Inter-rater• Have different people rate the “case”.

• Expressed as measures of rater agreement• Nominal (Kappa)• Categorical (Percent agreement, weighted Kappa )• Continuous (Correlation, ICC)

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Test Quality

• Diagnosis is an imperfect process - all tests have some inherent inaccuracy

• The “correct” diagnosis thus becomes a probability

• Understanding the mathematical performance of a test improves the clinicians decision making process.

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Measures of the Quality of a Diagnostic Test• Sensitivity• Specificity• Accuracy• Predictive Value (positive and negative)• The higher these numbers - the better the

test.

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the “Gold Standard”

• The definitive diagnostic technique• Often expensive, elaborate, or difficult to

perform.• We are always looking for faster, cheaper,

better ways to diagnose disease (and to determine treatment).

121

Sensitivity

• The number of people with the disease (Gold Standard) who have a positive test result.

• Relates Gold Standard to New Test.• A sensitive test rarely misses people with

disease.• Sensitive tests should be selected when there

is an important penalty for missing disease (i.e., cancer diagnosis)

122

Specificity

• The number of people without the disease who test positive.

• A specific test will rarely misclassify people without disease as diseased.

• Specific tests are used to “rule in” a diagnosis that has been suggested by other tests.

123

Accuracy of a Test

• The overall ability of a test to correctly classify a patient.

• Sensitivity + Specificity / 2

124

Predictive Value

• Positive predictive value is probability of disease in a patient with an abnormal test.

• Negative predictive value is the probability of no disease in a patient when the test result is normal.

125

A new diagnostic test for periodontal disease

126

“PERIOCHECK®”

• A new diagnostic assay that the company claims “predicts” future periodontal attachment loss (LOA).

• Requires a “blood test” of 1 ml of blood placed into the “Periocheck” machine.

• Values of the test range from -5 to +5• “Gold Standard” is actual attachment

loss (measured prospectively).

127

A Validation Study for PERIOCHECK

• 300 subjects recruited into study

• 2 edentulous exclusions

• 8 medical complication exclusions

• 4 refused upon consent

• 45% African Am• Mean age 49 ± 15y• Upon 2 year follow up

• 48 lost to follow up

• Final Study Sample• 238 (79%)

• 125 had LOA (52.5%)• 113 no LOA (47.5%)

128

Distribution of Baseline PERIOCHECK values by future LOA

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

People who do NOT develop LOA

People who DO develop LOA

Diagnostic Cutpoint ≥ 0

TN - True Negatives

TN

TP - True Positives

TP

FN - False Negatives

FN

FP - False Positives

FP

129

Distribution of Baseline PERIOCHECK values by future LOA

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

People who do NOT develop LOA

People who DO develop LOA

Diagnostic Cutpoint ≥ 0

TN - 91

TN

TP - 109

TP

FN - 16

FN

FP - 22

FP

Positive Test ≥ 0

Negative Test < 0

Disease Present

Disease Absent

Gold Standard (eventual LOA)

Periocheck

109 22

16 91

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

TN

TN

TP

TP

FN

FN

FP

FP

125 113 238

Prevalence = 125/238 = 52%

131

Quality of Diagnostic Test

• Sensitivity - the number of people with disease who have a positive test.

• Specificity - the number of people without a disease who have a negative test

Positive Test ≥ 0

Negative Test < 0

Disease Present

Disease Absent

Gold Standard (eventual LOA)

Periocheck

109 22

16 91

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

TN

TN

TP

TP

FN

FN

FP

FP

125 113 238

Sensitivity = 109/124 = 87.9%

Specificity = 91/113 = 80.5%

Prevalence = 125/238 = 52%

133

Performance related to “Cut Point”

• “cut point” is arbitrary and may be changed. • It is a decision point that a clinician may wish to

set for him/herself.• Sensitivity and Specificity are inversely

associated to one another and vary with the cut point

Positive Test ≥ 0

Negative Test < 0

Disease Present

Disease Absent

Gold Standard (eventual LOA)

Periocheck

109 22

16 91

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

TN

TN

TP

TP

FN

FN

FP

FP

125 113 238

Sensitivity = 109/125 = 87.9%

Specificity = 91/113 = 80.5%

Prevalence = 125/238 = 52%

Positive Test ≥ -2

Negative Test < -2

Disease Present

Disease Absent

Gold Standard (eventual LOA)

Periocheck

124 35

1 78

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

TN

TN

TP

TP

FN

FN

FP

FP

125 113 238

Sensitivity = 124/125 = 99.2%

Specificity = 78/113 = 69.0%

Prevalence = 125/238 = 52%

136

What we have so far

• That at the cut point studied (i.e., 0) • for every 100 patients without disease we

will correctly classify 80 of them. (Specificity)

• For every 100 patients with disease we will correctly classify 89 of them. (Sensitivity)

137

Relationship of Sensitivity/Specificity to Cut Point

Cut Point Sensitivity Specificity

-3 100 34

0 95 71

.5 90 82

1 83 91

3 55 99

138

ROC Curves

• Relates changes in sensitivity and specificity to changes in cut point.

• Provides overall utility of test• Suggests “optimal” cut point

139

Senst

1-Spec0

50

100

0 50 100

-20.5

1

1.5

3

ROC CURVE

140

Senst

1-Spec0

50

100

0 50 100

-10.5

1

1.5

2

ROC CURVE

141

Senst

1-Spec0

50

100

0 50 100

-10.5

1

1.5

2

ROC CURVE

142

Senst

1-Spec0

50

100

0 50 100

ROC CURVE

Area =.5

Area =.91

143

Senst

1-Spec0

50

100

0 50 100

ROC CURVE

Optimal cut point

144

What we actually get clinically• People with a “positive” test

• And we want to know how many really DO have disease

• Positive Predictive Value - the number of people with a positive test who have disease.

• People with a “negative” test• And we want to know how many really DO NOT have

disease.• Negative Predictive Value - the number of people

with a negative test who do not have disease.

Positive Test ≥ 0

Negative Test < 0

Disease Present

Disease Absent

Gold Standard (eventual LOA)

Periocheck

109 22

16 91

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

TN

TN

TP

TP

FN

FN

FP

FP

238

Positive Pred = 109/131 = 83.2%

Negative Pred = 91/107 = 85.0%

Prevalence = 125/238 = 52%

131

107

146

Test performance and prevalence

• Sensitivity and Specificity are stable properties

• PPV and NPV are frequency (Prevalence) dependent properties

Positive Test ≥ 0

Negative Test < 0

Disease Present

Disease Absent

Gold Standard (eventual LOA)

Periocheck

109 22

16 91

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

TN

TN

TP

TP

FN

FN

FP

FP

238

Positive Pred = 109/131 = 83.2%

Negative Pred = 91/107 = 85.0%

Prevalence = 125/238 = 52%

131

107

113125

Positive Test ≥ 0

Negative Test < 0

Disease Present

Disease Absent

Gold Standard (eventual LOA)

Periocheck

109 194

16 806

0

5

10

15

20

25

30

35

-4 -3 -2 -1 0 1 2 3 4

Periocheck Values

Fre

qu

ency

TN

TN

TP

TP

FN

FN

FP

FP

1125

Positive Pred = 109/303 = 35.9%

Negative Pred = 806/822 = 98.0%

Prevalence = 125/1125 = 11%

303

822

125 1000

149

Remember

• Sensitivity and Specificity are stable with changing prevalence, but will vary inversely with “cut point”.

• PPV/NPV vary by the prevalence of the population in which the test is administered.

• Best to use when uncertainty is high • Prevalence close to 50%

150

HIV Example (ELISA)When used in premarital screenings

• Sensitivity - 98• Specificity - 99• Prevalence - 250/100,000• PPV = 20%• 2 million marriages / year in US• HIV cases = 5,000• For every 1000 correctly diagnosed, there will

be 4000 false positives.

Research Ethics

• Subject safety• Informed Consent• Privacy and Confidentiality• Adverse events• Equipoise

151

Risk/Benefit RatioWritten Consent. IRB Approved. Full disclosure of Risks

how information is protected from unauthorized observation, and how participants are to be notified of any unforeseen findings from the research that they may or may not want to know.

The investigator must consider how adverse events will be handled; who will provide care for a participant injured in a study and who will pay for that care are important considerations.

the investigator should be in a state of "equipoise," that is, if a new intervention is being tested against the currently accepted treatment, the investigator should be genuinely uncertain which approach is superior.

Ethical Issues in Human Research

• Autonomy• Beneficence• Justice

152

the obligation on the part of the investigator to respect each participant as a person capable of making an informed decision regarding participation in the research study. The investigator must ensure that the participant has received a full disclosure of the nature of the study, the risks, benefits and alternatives, with an extended opportunity to ask questions.

Tuskegee: Study of syphilis in Blacks, without telling them of their participation. Deception and lack of informed consent used.Individuals followed for 40 years without treatment.

beneficence, which refers to the obligation on the part of the investigator to attempt to maximize benefits for the individual participant and/or society, while minimizing risk of harm to the individual. An honest and thorough risk/benefit calculation must be performed.

justice, which demands equitable selection of participants, i.e., avoiding participant populations that may be unfairly coerced into participating, such as prisoners and institutionalized children.

Components of Ethical, Valid Consent

• Disclosure• Understanding• Voluntariness• Competence• Consent

153

Disclosure: The potential participant must be informed as fully as possible of the nature and purpose of the research, the procedures to be used, the expected benefits to the participant and/or society, the potential of reasonably foreseeable risks, stresses, and discomforts, and alternatives to participating in the research.

Understanding: The participant must understand what has been explained and must be given the opportunity to ask questions and have them answered by one of the investigators.

Voluntariness: The participant's consent to participate in the research must be voluntary, free of any coercion or promises of benefits unlikely to result from participation.

Competence: The participant must be competent to give consent. If the participant is not competent due to mental status, disease, or emergency, a designated surrogate may provide consent if it is in the participant's best interest to participate.

Consent: The potential human subject must authorize his/her participation in the research study, preferably in writing, although at times an oral consent or assent may be more appropriate.

154

The End

Questions?