Chapter 1: The science and the scan

"Boring, But Necessary"

1. What is a PET/CT Scan?

Hybrid Imaging System
Anatomic & Functional Exam
The Machine
“Whole Body” vs. “Skull Base to Mid-Thigh”
Three Sets of Images
Produced

2. Basic Science 18F-FDG

Glucose Analog
Malignancy & Glucose Metabolism
Mechanisms for Increased Intracellular Glucose
Why 18F-FDG Works

3. Power of PET/CT

Whole Body Assessment
The “You’re Kidding Me!” Effect
Post-Therapeutic Scar vs. Active Malignancy

4. Indications for PET/CT

Detecting Malignancy
Staging Malignancy
Assess Response to Therapy
Detecting Recurrence

5. The Limitations of PET/CT

Not All Cancer is FDG-Avid
Normal FDG-Uptake vs. Pathologic Uptake
Technical Limitations
- Poor Patient Preparation
- Misregistration
- Brown Fat Activation
- SUV Problems
- Fields of View Discrepancy
- PET/CT Artifacts
- Timing of Exam After Therapy

6. Images Generated

CT Images
Non-Attenuation Corrected Images
Attenuation Corrected Images
Maximum Intensity Projection (MIP)
Fusion of Images
All Images Viewed in 3 Planes

7. Contrast Media: Oral & I.V.

Who Gets Oral Contrast?
Who Gets IV Contrast?
Oral Contrast “Cocktail” Recipe

8. What the Patient Should Expect

Documenting Height & Weight
Private Resting Room
Drinking PO Contrast
FDG Injection
Delay Between Injection & Scan

9. Safety Concerns with PET/CT Imaging

Radiation Exposure to Patient
Radiation Exposure to Patient’s Contacts
Patient Contact with Pregnant Women
Breastfeeding

Chapter 2: PET/CT Problems Which Limit Interpretation

"Something just doesn't seem right here"

1. Poor Patient Preparation

Optimizing Glucose & Insulin Levels
- Fasting Prior to Exam
- Diabetic Patients
- Low Carbohydrate Diet
- Hydration
Strenuous Exercise
Voiding Prior to Exam
Patient Instruction Sheet

2. Brown Fat

Definition
Distribution / Appearance
Don’t Miss the Hidden Nod
Reporting Language
Prevention

3. Timing of PET/CT Exam After Therapy

“Rule of 3”
- Chemotherapy: 1 month
- Surgery: 2 months
- Radiation: 3 months

4. Misregistration

Etiology: Hybrid Imaging
Patient Movement
Respiratory Motion
Breathing Techniques
Bowel Peristalsis

5. Extravasation of FDG

False Positives
False Negatives
Reporting Language

6. PET/CT Artifacts

Beam Hardening
Diaphragmatic Mismatch
Linear Hand Motion
Attenuation Correction
Differing Fields of View

7. The “Sponge Effect”

Poor Patient Preparation
FDG Extravasation
Extensive Brown Fat
Metformin-Induced Bowel Uptake
Marked Reactive Marrow Uptake
Extensive Tumor Uptake in

8. SUV Complications

Different Types of SUV Measurements
Factors that Influence SUV Measurements
What SUV Number Indicates Malignancy?
What Percent Change in SUV on a Follow Up Exam is Significant?
How to Compare Exams With Very Different Background Metabolic Activities?

Chapter 3: The Standardized Uptake Value (SUV)

"The good, the bad & the ugly"

1. What is the SUV & Why Used?

Quantitative vs. Qualitative Assessment
Unitless Measurement
Formula
SUV = ?

2. Variables that Affect SUV

Patient Preparation
Time Between FDG Injection & Scan
Partial Volume Effects
Extravasation
Patient Weight
Size & Position of ROI
Attenuation Correction Artifacts

3. Types of SUV Calculations

Consensus?
Body Weight
Lean Body Mass
Ideal Body Weight
Body Surface Area
Maximum vs. Mean
Average SUV’s by Organ

4. Interpreting the SUV: Threshold Values, “Oncologic Plausibility” & Relative Uptake

Precise Threshold Values?
“Oncologic Plausibility”
Relative Uptake
Assessing Nodes in Lymphoma Cases
Assessing Nodes in Non-Lymphoma Cases
Potential Lesions in Solid Organs
Pulmonary Nodules

5. What % Change in SUV on a Follow Up Exam is Clinically Significant?

The Problem
Current Recommendations

6. How to Compare Sequential Exams With Very Different Background Activities?

Differing Background Metabolic Activities
When Qualitative Assessment is Required
Reporting Language

7. Should We Just Abandon the SUV?

Pros & Cons
“Qualitative” Definitions
- Mild
- Moderate
- Intense
Final Recommendations

Chapter 4: Our Systematic Approach to Reading a PET/CT

"Eat your vegetables"

1. Reading Station & Reading Software

Reading Station
Monitor Set-Up
PET/CT Reading Software
Hanging Protocol

2. General Reading Caveats

Reading in Context (“Oncologic Plausibility”)
Measure Size on CT, Not on PET Images
Abnormality Seen Only on First PET Image
Assess the Patient’s Main Pathology Last
Beware the Ureter

3. Excellent Views: The MIP, Coronal & Sagittal Images

3-D Rotating MIP & Coronal “Quick MIP”
Coronal PET
Sagittal PET

4. Written Annotations While Reading

Numbers, Numbers & More Numbers
Size & SUV Annotation System
Sample Annotation Sheet

5. The Language of Reporting

Goals of Reporting
Lawyers, Lawyers & Lawyers
Sample PET/CT Report
- Negative Exam
- Positive Exam
Patient Questionnaire
Technologist’s Data Sheet

6. The Read

Huge Exam: Requires Systematic Approach
Our “12-Step Reading System”
“The Read” in Action: Sample Case (Video)
Annotations for Sample Case
Final Report for Sample Case

Chapter 5: Normal Physiologic Distribution of FDG

"The essentials"

1. Introduction

To Locate Cancer, First Eliminate:
- Normal FDG-Avid “Structures”
- Benign FDG-Avid “Findings”

2. Head & Neck

3. Chest

4. Abdomen

5. Pelvis

6. Miscellaneous

Gastrointestinal Stromal Tumor (GIST)

Fast Facts:

≈ 3% of all GI cancers (≈ 20% of small bowel cancers)
Can occur anywhere along GI tract:
- Stomach (≈ 65%)
- Small Bowel (≈25%)
- Uncommon: rectum, esophagus, colon, appendix

Role of PET/CT in the Management of GIST:

PET/CT plays a very important role in the management and evaluation of GIST patients.

Surgical resection is the goal for patients with resectable lesions and no evidence of metastatic disease. The mainstay of medical therapy is Imatinib, a protein kinase inhibitor (GIST are generally resistant to both chemotherapy and radiation).

The vast majority of GIST lesions (≈ 85%) respond extremely rapidly to Imatinib therapy. This response, however, is often not accompanied by a decrease in lesion size until very late in therapy.

PET/CT, therefore, plays a unique role in the early assessment of therapy response to Imatinib, as it can demonstrate a significant decrease in a lesion’s metabolic activity, even though the lesion may be unchanged in size (in fact, some lesions may actually increase in size during successful treatment, presumably due to inflammation and/or hemorrhage).

PET/CT is regularly utilized for:

Initial Staging:

Primary lesion: Size, location and metabolic activity.
Metastatic disease: Present ≈ 10% at time of diagnosis – typically to the liver, omentum, & peritoneum (nodes, bone & lung involvement are less common).

Assessing Response to Therapy & Prognosis:

Early Response: Non-responders can be offered alternative therapy.
Late Response: Assess success or failure of therapy, and ultimate outcome. Can also assess secondary resistance to Imatinib.

Recurrence & Restaging:

Restaging suspected recurrence.
Distinguishing recurrence from post-therapeutic inflammation.

Criteria for “Active Malignancy”:

Most patients with GIST patients already have a biopsy-proven diagnosis prior to PET/CT scanning. Occasionally, however, an incidental GIST is encountered.

GIST lesions generally present as an FDG-avid soft tissue mass, typically involving the stomach or small bowel (we usually do not specifically include GIST in our differential for FDG-avid colon, rectal, esophageal or appendiceal lesions).

Larger lesions are often accompanied by cystic regions, often representing necrosis.

Recurrent Active Disease: Often appears as a small focus of activity within a larger non-avid treated mass (the recurrence may be centrally or peripherally located).

False Positives:

“Flare Phenomenon”: Within the first 3 weeks after cessation of Imatinib therapy, there is often a transient increase in the metabolic activity of residual lesions. For this reason, we generally suggest post-treatment imaging be delayed for at least 6 weeks.