Pittsburgh Compound B (PiB)

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Pittsburgh Compound B (PiB)

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Overview

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Overview

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Pittsburgh Compound B (PiB), chemically known as [N-methyl-11C]2-(4'-methylaminophenyl)-6-hydroxybenzothiazole, is a PET radiotracer developed at the University of Pittsburgh that binds to amyloid-beta (Abeta) plaques in the brain. It was the first amyloid PET tracer and remains a gold standard for amyloid imaging in Alzheimer's disease research. Since its first human use in 2002, PiB has been fundamental in advancing our understanding of amyloid pathology in living humans and has enabled critical studies on disease progression, biomarker validation, and therapeutic trials. [@klunk2004]

Historical Development

Origins of Amyloid PET Imaging

Before PiB, amyloid pathology could only be assessed postmortem through autopsy or biopsy. The development of PiB represented a paradigm shift, allowing visualization of amyloid plaques in living patients. The tracer was designed based on the thioflavin-T structure, which had long been known to bind to amyloid fibrils in histological staining. [@klunk2004]

The key innovations that made PiB suitable for human PET imaging included:

Blood-brain barrier penetration: The lipophilic nature of PiB enables rapid brain uptake

High affinity for fibrillar Aβ: The Kd for amyloid plaques is approximately 0.8 nM

Specific binding: Minimal off-target binding in the brain

Suitable half-life: Carbon-11 labeling allows dynamic imaging protocols

Development Timeline

| Year | Milestone | Reference |
|------|-----------|------------|
| 2002 | First human PET studies | Mintun et al., 2006 |
| 2004 | Initial validation publication | Klunk et al., 2004 |
| 2007 | Large cohort AD/MCI imaging | Rowe et al., 2007 |
| 2013 | Centiloid scale established | Jack et al., 2013 |
| 2018 | NIA-AA framework integration | Jack et al., 2018 |

Mechanism of Action

Chemical Properties

PiB is a derivative of thioflavin-T, modified to optimize its pharmacokinetic properties for PET imaging. The key structural features include: [@klunk2004] [@schreiber2018]

Benzothiazole core: Provides high affinity for amyloid fibrils
N-methyl group: Improves brain uptake kinetics
Hydroxyl group: Enhances specific binding to Aβ plaques

Binding Characteristics

PiB binds with high affinity to: [@villain2009]

Fibrillar amyloid-beta: Both Aβ40 and Aβ42 plaques

Core of neuritic plaques: The dense core regions show highest binding

Vascular amyloid: Cerebral amyloid angiopathy (CAA) deposits

The binding is specific to the cross-beta sheet structure characteristic of amyloid fibrils, which explains why PiB shows minimal binding to diffuse Aβ deposits that lack this organized structure.

Kinetics and Distribution

The pharmacokinetics of PiB follow a characteristic pattern: [@rowe2007] [@mintun2006]

| Phase | Time | Characteristics |
|-------|------|----------------|
| Rapid uptake | 0-5 min | Peak brain delivery, high blood clearance |
| Early equilibrium | 5-15 min | Initial distribution throughout brain |
| Specific binding | 30-60 min | Progressive retention in amyloid-rich regions |
| Washout | 60-90 min | Non-specific binding clears, specific remains |

Clinical Validation

Diagnostic Performance

PiB PET has demonstrated excellent diagnostic performance in numerous clinical studies: [@jack2013] [@johnson2016]

| Clinical Scenario | Sensitivity | Specificity | AUC |
|-------------------|-------------|-------------|-----|
| AD vs. healthy controls | 85-95% | 85-95% | 0.92-0.96 |
| AD vs. other dementias | 75-90% | 60-80% | 0.75-0.85 |
| MCI converters to AD | 80-90% | 70-85% | 0.80-0.88 |

Regional Distribution Patterns

The characteristic PiB retention pattern in AD follows the known distribution of amyloid pathology: [@villain2009]

Highest uptake regions: Prefrontal cortex, precuneus, posterior cingulate cortex, and orbitofrontal cortex
Intermediate uptake: Lateral temporal cortex, parietal cortex, and hippocampus
Lowest uptake: Primary motor cortex, sensory cortex, cerebellum (except for cerebellar amyloid in advanced cases)

This regional pattern aligns with the staging scheme proposed by Thal and colleagues, where amyloid deposition follows a characteristic progression from neocortical to allocortical and finally to brainstem regions.

Correlation with Neuropathology

Postmortem studies have validated PiB binding against neuropathological assessments: [@schreiber2018] [@bucci2019]

Strong correlation: PiB retention correlates with neuritic plaque density (r = 0.7-0.85)
Moderate correlation: PiB shows weaker correlation with diffuse Aβ plaques
CAA correlation: PiB effectively detects cerebrovascular amyloid

Standardized Uptake Value Ratio (SUVR)

Quantification Methods

SUVR calculation uses a reference region to normalize PiB uptake: [@bullich2018]

Common reference regions:

Cerebellar gray matter (most common in research)
Whole cerebellum
Pons (in some early studies)
Subcortical white matter

Centiloid Scale:

The centiloid scale was developed to standardize PiB measurements across different studies and scanners: [@jack2013]

| Centiloid Value | Interpretation |
|-----------------|----------------|
| 0 | Mean of young controls (age <45) |
| 100 | Mean of typical AD patients |
| >100 | High amyloid burden |
| <20 | Amyloid negative |

Cutoff values:

SUVR >1.4-1.5 (cerebellar reference): Amyloid positive
Centiloid >20-30: Amyloid positive

Quality Control Considerations

Several technical factors can affect SUVR quantification: [@bullich2018]

Partial volume effects: Corrections needed in atrophic brains

Scan duration: 30-90 minute frames recommended

Reconstruction parameters: Standardized protocols essential

Motion artifacts: Quality control critical for reliable results

Clinical Applications

Research Applications

PiB PET has transformed Alzheimer's disease research in multiple ways: [@mathis2013] [@collins2019]

Biomarker validation: Enabled validation of CSF and blood biomarkers against in vivo amyloid

Natural history studies: Characterized preclinical AD progression

Trial enrichment: Identified amyloid-positive participants for clinical trials

Genetic studies: GWAS identified variants affecting brain amyloid deposition

Disease modeling: Informed computational models of AD progression

Clinical Use Indications

Amyloid PET (including PiB) is clinically indicated in specific scenarios: [@feldman2020] [@johnson2016]

Atypical dementia presentations: When diagnosis is unclear
Early-onset dementia: Age <65 with unclear etiology
Differential diagnosis: Distinguishing AD from FTLD, DLB, vascular dementia
Clinical trial enrollment: Confirmation of amyloid pathology

Impact on Clinical Management

Studies have shown that amyloid PET results: [@morris2016] [@logan2020]

Change diagnosis: Alters clinical diagnosis in 20-30% of cases
Affect treatment: May lead to changes in pharmacological management
Inform prognosis: Provides prognostic information for MCI patients
Reduce uncertainty: Decreases diagnostic uncertainty for clinicians and families

Comparison to Other Amyloid PET Tracers

PiB was the first amyloid PET tracer, but several F-18 labeled tracers are now FDA-approved for clinical use: [@seibyl2016] [@sabri2015]

| Tracer | Half-life | Clinical Status | Advantages |
|--------|-----------|-----------------|-------------|
| PiB (C-11) | 20 min | Research only | Highest affinity, research gold standard |
| Florbetapir (Amyvid) | 110 min | FDA approved | Widely available, practical |
| Florbetaben (Neuraceq) | 110 min | FDA approved | High specificity |
| Flutemetamol (Vizamyl) | 110 min | FDA approved | Similar to PiB |

PiB vs. F-18 Tracers Comparison

| Property | PiB | F-18 Tracers |
|----------|-----|--------------|
| Half-life | 20 min | 110 min |
| Production | On-site cyclotron | Generator-produced |
| Scan time | 40-60 min | 20 min |
| Signal-to-noise | Excellent | Good |
| Clinical availability | Research only | FDA approved |

The shorter half-life of C-11 requires on-site cyclotron production, limiting PiB use to major research centers. F-18 tracers can be distributed from central production facilities, enabling broader clinical access.

Biological Insights from PiB Studies

Amyloid Deposition Trajectories

PiB studies have characterized the natural history of amyloid deposition: [@jack2013] [@jack]

Preclinical phase: Amyloid accumulates 15-20 years before clinical symptoms
Nonlinear progression: Rapid accumulation in early stages, slower later
Plateau phase: Amyloid levels plateau in clinical AD stages

Factors Affecting PiB Retention

Multiple factors influence PiB uptake beyond amyloid: [@hatton2015] [@collins2019]

Age: Older individuals show higher PiB retention

APOE genotype: APOE ε4 carriers show higher and earlier PiB retention

Sex: Some studies show sex differences in amyloid accumulation

Vascular pathology: Confounding effects in mixed pathology cases

Cognitive Correlations

PiB retention shows characteristic relationships with cognitive measures:

Threshold effect: Cognitive impairment only manifests once amyloid reaches a threshold
Regional specificity: Posterior cingulate PiB shows strongest cognitive correlations
Interaction effects: Amyloid and tau show synergistic effects on cognition

PiB in Special Populations

Down Syndrome

Individuals with Down syndrome have a high prevalence of Alzheimer's-type pathology due to the extra copy of the APP gene located on chromosome 21. PiB studies in Down syndrome have revealed: [@hatton2015]

Early amyloid deposition: Amyloid accumulation begins in the third decade of life
Trisomy 21 effect: The APP gene triplication leads to accelerated Aβ production
Clinical correlates: PiB retention correlates with cognitive decline in adults with DS
Diagnostic challenges: Distinguishing AD from DS-related cognitive changes

Autosomal Dominant AD

PiB has been extensively used in studies of familial AD caused by mutations in APP, PSEN1, and PSEN2:

Preclinical detection: Abnormal PiB retention 10-15 years before expected onset
Mutation-specific patterns: Different mutations show varying regional patterns
Age at onset prediction: PiB levels help estimate age of clinical onset
Clinical trial applications: Identifying mutation carriers for preventive trials

Mild Cognitive Impairment

PiB PET is particularly valuable in MCI patients: [@logan2020]

Conversion prediction: PiB-positive MCI patients have higher conversion rates to AD
Prognostic information: Helps identify which MCI patients will progress
Treatment targeting: Identifies amyloid-positive MCI for anti-amyloid therapies
Biomarker combinations: Best predictive models combine PiB with tau PET or CSF

Limitations

Despite its revolutionary impact, PiB has several limitations: [@bucci2019]

Technical Limitations

Short half-life: Requires on-site cyclotron (C-11 only)

Production costs: Complex radiosynthesis limits availability

Scan duration: Longer than F-18 tracers

Quantification complexity: Requires careful standardization

Scanner variability: Different scanners and reconstruction methods can affect results

Motion sensitivity: Longer scans increase susceptibility to motion artifacts

Partial volume effects: Brain atrophy can cause underestimation of true retention

Biological Limitations

White matter binding: Non-specific binding in white matter can confound analysis

Not disease-specific: Positive in other conditions with amyloid (CAA, DLB)

Limited sensitivity to diffuse plaques: Prefers fibrillar over diffuse Aβ

Floor effects: Cannot detect low-level amyloid in amyloid-negative individuals

Vascular amyloid interference: Cerebral amyloid angiopathy contributes to signal

Off-target binding: Specific binding to melanin in some brain regions

Age-related changes: Normal aging associated with subtle increases in retention

Clinical Limitations

Cost: More expensive than CSF biomarkers

Accessibility: Limited to major research centers

Radiation exposure: Ionizing radiation from PET imaging

Insurance coverage: Limited CMS coverage in the US

Availability: Not FDA approved, restricting clinical use

Turnaround time: Results take days to weeks in research settings

Interpretation Challenges

Several factors can complicate PiB interpretation:

Borderline cases: Some individuals show intermediate centiloid values

Mixed pathologies: Co-existing tau, vascular, or Lewy body pathology

APOE effects: APOE ε4 carriers may show different retention patterns

Education effects: Cognitive reserve can modify clinical manifestations

Technical artifacts: Need for careful quality control

Technical Considerations for PiB PET

Image Acquisition Protocols

Standard PiB PET imaging protocols include: [@bullich2018]

| Parameter | Recommendation |
|-----------|----------------|
| Tracer dose | 370-555 MBq (10-15 mCi) |
| Scan duration | 50-70 minutes post-injection |
| Frame structure | Multiple dynamic frames (4 × 5 min) |
| Attenuation correction | CT or transmission scan |
| Reconstruction | OSEM or filtered backprojection |

SUVR Calculation Best Practices

For reliable SUVR measurements:

Frame selection: Use late frames (40-70 min) for optimal signal

Reference region choice: Cerebellar gray matter preferred

Partial volume correction: Apply in atrophic brains

Harmonization: Use centiloid for cross-study comparisons

Quality control: Review images for motion and artifacts

Longitudinal Monitoring

PiB PET is useful for tracking amyloid changes over time:

Annual change: Typical rate of 1-3 centiloids per year in AD
Plateau effect: Rates decrease in later disease stages
Treatment effects: Anti-amyloid drugs show 20-40 centiloid reductions
Variability: Test-retest reliability is approximately 5%

Regional PiB Patterns in Different Conditions

Typical AD Pattern

PiB retention in AD shows a characteristic regional hierarchy:

Highest: Precuneus, posterior cingulate, prefrontal cortex

High: Orbitofrontal, lateral temporal, parietal cortex

Moderate: Hippocampus, amygdala, thalamus

Low: Brainstem, cerebellar cortex, primary sensory regions

Atypical Patterns

Different AD clinical variants show distinct patterns:

| Variant | PiB Pattern |
|---------|-------------|
| Posterior cortical atrophy | Occipital > frontal |
| Logopenic PPA | Left temporoparietal |
| Corticobasal syndrome | Asymmetric frontal/parietal |
| Primary progressive aphasia | Language dominant hemisphere |

Non-AD Conditions

PiB positivity can occur in:

Lewy body disease: Variable positivity (30-50%)
Cerebral amyloid angiopathy: Posterior regions
Down syndrome: Similar to AD pattern
Some controls: Low-level positivity in elderly

Regulatory Status

United States

PiB (C-11): Research use only, not FDA approved
Florbetapir (Amyvid): FDA approved in 2012
Flutemetamol (Vizamyl): FDA approved in 2013
Florbetaben (Neuraceq): FDA approved in 2014

Europe

PiB: Available in research settings
Florbetapir: EMA approved
Flutemetamol: EMA approved
Florbetaben: EMA approved

Coverage

CMS: Amyloid PET covered for specific clinical scenarios (Medicare Coverage of Innovative Technologies)
Private insurers: Variable coverage policies
Research: Funded by NIH and private foundations

Future Directions

Quantitative Improvements

PVE corrections: Improved partial volume effect corrections using MRI-based segmentation
Dynamic modeling: Kinetic modeling approaches for better quantification
Centiloid standardization: Universal adoption of the centiloid scale
Harmonization: Cross-scanner and cross-site standardization protocols
Machine learning: Automated quantification and interpretation

Multi-Modal Integration

PET/MRI: Combined imaging for structural and molecular correlation
PET/tau: Simultaneous amyloid and tau imaging
Blood-amyloid correlation: Integration with blood-based biomarkers
Multimodal prediction: Combining PiB with genetic, cognitive, and CSF data
Amyloid PET in drug development: Tracking anti-amyloid treatment effects

Therapeutic Applications

Anti-amyloid monitoring: Tracking amyloid reduction in treatment trials
Dose-response: Correlating drug exposure with amyloid changes
Biomarker-guided treatment: Personalized medicine approaches
Combination therapies: Monitoring multiple pathological targets
Preclinical trials: Identifying optimal treatment windows

Related Biomarkers

[Amyloid-beta 42/40 ratio](/biomarkers/amyloid-beta-42-40-ratio) - CSF amyloid marker
[CSF p-tau 181](/biomarkers/p-tau-181) - Tau pathology marker
[Florbetapir (Amyvid)](/biomarkers/florbetapir) - F-18 amyloid PET
[Tau PET imaging](/biomarkers/tau-pet-imaging) - Tau pathology imaging
[Amyloid PET imaging](/biomarkers/amyloid-pet-imaging) - General amyloid imaging

Key Research Papers

Klunk et al., 2004 (PMID:15501088) - Original PiB development and validation

Rowe et al., 2007 (PMID:17630852) - Large cohort AD and MCI imaging

Jack et al., 2013 (PMID:24136952) - Centiloid scale development

Johnson et al., 2016 (PMID:26764621) - Clinical utility of amyloid PET

Morris et al., 2016 (PMID:27174384) - Impact on clinical outcomes

Schreiber et al., 2018 (PMID:29454756) - Postmortem correlation studies

Villain et al., 2009 (PMID:19159241) - Regional distribution patterns

Bullich et al., 2018 (PMID:29338902) - SUVR quantification best practices

External Links

[PubMed - PiB PET Studies](https://pubmed.ncbi.nlm.nih.gov/?term=Pittsburgh+Compound+B+PiB+PET+Alzheimer)
[Alzheimer's Disease Neuroimaging Initiative (ADNI)](https://adni.loni.usc.edu/)
[Centiloid Project](https://www.gaain.org/centiloid-project)
[University of Pittsburgh PiB Development](https://www.pitt.edu/) - Original PiB development center

References

bucci2019, Molecular imaging of amyloid in vivo (2019) (2019)
bullich2018, Amyloid PET SUVR quantification (2018) (2018)
collins2019, Amyloid PET and CSF biomarkers (2019) (2019)
feldman2020, Amyloid PET in clinical practice (2020) (2020)
forman2006, Reduced PiB binding in cognitively normal (2006) (2006)
hatton2015, Amyloid PET imaging in Down syndrome (2015) (2015)
jack, NIA-AA Framework for AD biomarkers
jack2013, Age-related trajectories of amyloid PET (2013) (2013)
jack2018, NIA-AA research framework update (2018) (2018)
johnson2016, Diagnostic utility of amyloid PET (2016) (2016)
klunk2004, The binding of PiB to amyloid plaques (2004) (2004)
logan2020, Amyloid PET in mild cognitive impairment (2020) (2020)
mathis2013, Amyloid PET imaging in Alzheimer's disease (2013) (2013)
mintun2006, [C-11]PiB PET in AD patients (2006) (2006)
morris2016, Impact of amyloid PET on cognitive outcomes (2016) (2016)
rowe2007, PiB PET imaging in AD and MCI (2007) (2007)
sabri2015, Florbetaben F 18 PET imaging (2015) (2015)
schreiber2018, PiB retention in human brain (2018) (2018)
seibyl2016, PET imaging of beta-amyloid with florbetapir F 18 (2016) (2016)
villain2009, Regional distribution of PiB in Alzheimer's disease (2009) (2009)

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derives_from?Multimodal prediction90%

derives_from?Combination therapies90%

derives_from?Harmonization90%

derives_from?Blood-amyloid correlation90%

derives_from?Amyloid PET in drug development90%

derives_from?Preclinical trials90%

derives_from?Machine learning90%

derives_from?PVE corrections90%

derives_from?Anti-amyloid monitoring90%

derives_from?Dynamic modeling90%

derives_from?Dose-response90%

derives_from?Biomarker-guided treatment90%

derives_from?Centiloid standardization90%

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