PANEL DISCUSSION – INDIAN PERSPECTIVE

1. PANEL DISCUSSION – INDIAN PERSPECTIVE • Das Gupta, MD, PhD Super Religare Laboratories

2. Points for discussion • QA • Tests offered by SRL • Practical issues • Potential areas of collaboration

3. TESTS OFFERED BY SRL • Lymphocyte subset enumeration (T, B & NK) (2-colour, 3-colour, 4-colour) • Leukemia/lymphoma immunophenotyping • PNH diagnosis by RBC analysis • HLA B27 typing • Zap 70 • DNA/Cell cycle analysis

4. ISSUES General issues • Cost – Instrument upgrading (multicolour assays), Reagent cost, “Ideal” (often large) panels • Validation • Trained manpower • Distant testing Specific issues • DNA/Cell cycle analysis Review indications (Hematolymphoid, Solid tumours) Standardize assay • MDS diagnosis Need for each lab to develop its own data on normal antigenic profile of hematopoietic cells

5. Strategy for Two-colour Pan LeucoGating-CD4 Count

6. Correlation of CD4 lymphocyte counts by Tetrachrome and PLG-CD4 reagent

7. Conclusion 1 CD4 lymphocyte counts obtained by PLG-CD4 (2-colour) reagent (one-third cost) showed a high degree of correlation with those obtained by more expensive Tetrachrome (4-colour) reagent

8. Stability of CD4 counts in EDTA

9. Stability of CD4 counts in heparin

10. Conclusion 2 • Suitability of anticoagulants For two colour CD4 enumeration using Pan LeucoGating (PLG) strategy heparin was found to be as good an anticoagulant for distant testing as EDTA (48 hrs). • Allowable time since collection Forty-eight hrs in EDTA and Heparin

11. Correlation between CD4 counts obtained by using full and half volume reagents

12. Conclusion 3 Excellent correlation was observed between CD4 lymphocyte subset counts obtained by using the recommended volume of reagents and those obtained by half the recommended volume

13. POTENTIAL AREAS OF COLLABORATION • Zap 70 assay standardization • Immunodeficiency panels • Wider and more organized PT programme • Sharing of patient data and other information • Role of premier (teaching) institutions and reference laboratories

14. Thank you

16. Proposed Scoring System for Immunophenotypic Distinction between Acute Myelogenous Leukemia with Thymic (T) Markers and T-Acute Lymphoblastic Leukemia with Myeloid Markers A. Das Gupta, M. Ramani, A. Vazifdar and V. Mehrotra Super Religare Laboratories, India

17. Background • A commonly observed example of expression of trans-lineage markers by blast cells in AL is the expression of T lymphoid markers by myeloblasts in AML (20-40%) [AML(T)] Conversely, 20-30% of T-ALL cases express myeloid markers [T-ALL(M)]. • An accurate distinction between these two entities using commonly applied primary antibody panels is a significant challenge. • Even the use of an advanced software (Infinicyt) and EuroFlow ALOT that includes cytoplasmic markers was not able to correctly classify >3% (5/157) cases of AL. All these cases had an overlapping myeloid and T-lymphoid phenotype.

18. APS (Automated Population Separation) : Unsupervised classification of the different leukemias by principal component analysis (PCA). Based on the ALOT combination, all typical cases of AL (152/157) can be recognized with the new approach. No case was misclassified.

19. Five atypical cases of AL clustered together either in an area comprised between AML and T-ALL cases, or at the bottom of the 2 clusters. There was no equivalent B/AML overlap.

20. Therefore, there is a need for identifying immunophenotypic features of blast cells in these two conditions and develop a method/system that will allow distinction between these two entities.

21. Four-Colour Primary Antibody Panel Used

22. Results

23. COMPARISON OF EXPRESSION OF LINEAGE-ASSOCIATED MARKERS IN AML(T) AND IN T-ALL(M)

24. All cases of T-ALL with or without myeloid marker expression had a score of =/<3.5 • All cases of AML with or without T-lymphoid markers had a score =/>4.5 • Cases of true mixed lineage leukemia had a score between 3.5-4.5

25. We have applied the scoring system in a prospective manner to test its power in predicting the correct diagnosis. • We are refining the scoring system further by adopting statistical methods.

26. Something more…..

27. A. Das Gupta, M. Ramani, V. Mehrotra and A. Vazifdar Super Religare Laboratories, India Panel Discussion – Some Issues in Lymphocyte Subset Enumeration…

28. Issues in Lymphocyte Subset Enumeration Cost-related Issues • Cost-effective CD4+ lymphocyte subset enumeration (two colour reagent vs 3-4 colour reagent) • Use of lower volume of reagents per assay Issues of distance testing Transit time in distant testing scenario – allowable time from sample collection and suitability of anticoagulants

29. Issues in Lymphocyte Subset Enumeration Cost-related Issues • Cost-effective CD4+ lymphocyte subset enumeration (two colour reagent vs 3-4 colour reagent) • Use of lower volume of reagents Issues of distance testing Transit time in distant testing scenario – allowable time from sample collection and suitability of anticoagulants

30. Issues in Lymphocyte Subset Enumeration Cost-related Issues • Cost-effective CD4+ lymphocyte subset enumeration (two colour reagent vs 3-4 colour reagent) • Use of lower volume of reagents Issues of distance testing Transit time in distant testing scenario – allowable time from sample collection and suitability of anticoagulants