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Grading Systems for CTA Rejection Proposals and Prospects

Grading Systems for CTA Rejection Proposals and Prospects. David E. Kleiner, M.D., Ph.D. National Cancer Institute. Setting the Stage. Grading system philosophy and choices of grading systems Review of published grading system criteria for CTA acute rejection

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Grading Systems for CTA Rejection Proposals and Prospects

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  1. Grading Systems for CTA RejectionProposals and Prospects David E. Kleiner, M.D., Ph.D. National Cancer Institute

  2. Setting the Stage • Grading system philosophy and choices of grading systems • Review of published grading system criteria for CTA acute rejection • Comparison of existing systems looking for common themes • Where do we go from here?

  3. What Are the Goals in Creating a Grading System? • Stratification for treatment/protocol entry • Minimum hepatic fibrosis for HCV therapy • Prognostication • Cancer Staging and Grading • Structured pathology data collection • NASH-CRN Feature Scoring System

  4. Some Definitions • Stage – Stratification of the level of progress of a disease to its final end-point (Clinical Tool) • Grade – Stratification of the severity of a disease or disease feature at a particular point in time (Clinical Tool) • Scoring – the assignment of quantitative or semi-quantitative values to individual disease features (Research Tool) It is usually possible for therapeutic intervention to improve the Grade of a disease but it is usually difficult or impossible to improve the Stage of a disease

  5. Organ Failure Cirrhosis Loss of Function (Stage) Rate (Grade) The apparent rate may or may not be a good predictor of progression Onset of Disease Death Time

  6. Types of Grading Systems • Tiered Systems • Each grade is differentiated by the addition of a new lesion • Banff Renal Acute Cellular Rejection Grade I vs II • Progressive Severity Systems • Gradual worsening of one or more features with (arbitrary) thresholds • Banff Renal Acute Cellular Rejection Borderline vs Ia vs Ib • Composite Score Systems • Grade is a summation of scores of individual features • Hepatitis inflammation grading

  7. Tiered Grading Systems • Advantages: Easy to use, Probably better reproducibility • Disadvantages: Doesn’t account well for variation in severity of features, especially when features seem inappropriately mild or negative

  8. Progressive Severity System • Advantages: Better system when features generally vary in parallel. Natural relationship to scoring individual features • Disadvantages: Need to define thresholds for each feature -> decreases reproducibility. Difficulties assigning grade if features are out of sync with one another.

  9. Composite Score System Sum the individual scores:0: Grade 0; 1-3: Grade 1; 4-6: Grade 2; 7-9: Grade 3 • Advantages: Most sophisticated system. Accounts well for individual variation between features. Relates well to scoring systems. Better for clinical trials • Disadvantages: Threshold problems. Implied weighting of features, therefore requires advanced knowledge of relative importance of features

  10. Published Systems for Grading CTA Rejection • The Pathology of Full Thickness Cadaver Skin Transplant for Large Abdominal Defects • Bejarano et al., Am. J. Surg. Pathol. 28: 670-675; 2004 • Steroid- and ATG-Resistant Rejection After Double Forearm Transplantation Responds to Campath-1H • Schneeberger et al., Am. J. Transplant 4: 1372-1374; 2004 • Pathological Score for the Evaluation of Allograft Rejection in Human Hand (Composite Tissue) Allotransplantation • Kanitakis et al., Eur J. Dermatol. 15: 235-8; 2005 • Composite Tissue Allotransplantation: Classification of Clinical Acute Skin Rejection • Cendales et al., Transplantation 81:418-22; 2006

  11. Abdominal wall transplantation • 9 patients (5 adults, 4 children), 10 transplants • 22 specimens (17 punch biopsies, 3 graft excisions, 2 post-mortem) • Blind categorization (3 pathologists) of multiple histologic features related to inflammation, epidermal changes and stromal changes • Features were analyzed with respect to an overall clinico-pathologic determination of the presence of rejection

  12. Histologic Associations with Rejection

  13. Case report of 41 M with double forearm transplantation • Grading system presented based on clinical experience with prior rejection episodes and on published literature of CTA rejection • Reported 2 Grade I rejections that were steroid-responsive and one Grade IVa rejection that was steroid-resistant and ATG-resistant but responded to Campath-1H • Follow-up biopsies confirmed resolution of infiltrates

  14. Hand/Forearm Transplants • 6 patients (all M), 33.8 yrs (22-48) • 89 skin biopsies (punch or scalpel) • Biopsies reviewed for a variety of epidermal, adnexal, inflammatory and vascular changes • Immunoperoxidase staining for lymphocyte phenotype, HLA, mast cells • Grading based on biopsy review, grouping similar biopsies together into 5 grades

  15. Forearm transplantation • 2 patients, 11 biopsies • Biopsies were ranked by overall severity of changes and grouped into categories to set definitions • Interobserver agreement tested on grading 18 additional biopsies from abdominal wall transplants

  16. Common Themes • Perivascular lymphocytic infiltrates become progressively more intense and involve more vessels with increasing grades • Inflammation extends to involve dermal stroma, epidermis (including DEJ), adnexa at moderate to marked grades • Epidermal apoptosis/necrosis only at higher grades • All tiered grading systems with implied worsening inflammation with increasing grade

  17. Grades from None/Non-specific to Mild/Moderate Proposal 1st author: 1. Bejarano, 2. Schneeberger, 3. Kanitakis, 4. Cendales

  18. Grades from Moderate to Very Severe Proposal 1st author: 1. Bejarano, 2. Schneeberger, 3. Kanitakis, 4. Cendales

  19. Approximate Grade Equivalences

  20. Conclusions and Challenges • There is already substantial agreement on basic grade stratification for acute rejection • Histologic features of rejection (especially at mild grades) are also seen in a large variety of non-rejection pathologies • Published experience using pathology grading in prospective studies is very limited • Future refinements may require prospective systematic evaluation of biopsy features, similar to other developed rejection classification systems • We should consider defining scoring thresholds for scaling individual features (inflammation, epidermal injury etc.)

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