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Chronic rejection- current
concepts and newer perspectives

        Kim Solez, M.D.
Mentor influences: Smelling the Flowers
    Meetings – Not A Waste of Time!
   “You should take time to smell the flowers.” (1972)
   “Medical meetings are just social events. Nothing important happens at
    them. They are a waste of time. You should avoid organizing medical
    meetings.” - Robert H. Heptinstall, M.D.
   I did not follow the latter advice. Physicians need to be socialized,
    humanized. Organized my first Acute Renal Failure Symposium in 1982,
    published as a book in 1984 Acute Renal Failure: Correlations Between
    Morphology and Function. Many other meetings since then. Banff
    meetings began 1991, continued every two years since then.
   Technology and Future of Medicine course began 2011, mixes science
    and humanities, technological Singularity, futurism, exponential change.
   High impact education changes human behavior, like advertising does. In
    the area of late biopsies and the scarred allograft in Banff consensus
    process we have been working to change behavior for some time.
   Evolution of thinking from chronic rejection, to chronic allograft
    nephropathy, to interstitial fibrosis and tubular atrophy.
An Evolution in Which We Find Evidence of the
     Human Tendency to Try to Believe in Specific Entities
     There Is No Evidence For!
   Originally all late scarring processes in the transplanted kidney were
    called “chronic rejection”.

   In order to stop perpetuating the idea that everything was chronic rejection
    we coined the term “chronic allograft pathology” – “CAN” for these
    nonspecific chronic changes.

   People seized on CAN as a new entity, devised strategies to prevent it,
    animal models for it etc. Soon there were hundreds of articles about CAN.

   To stop this artificial glorification of nonspecific changes as a new entity
    we eliminated the phrase CAN and used the descriptive terms interstitial
    fibrosis and tubular atrophy instead - IFTA.
Number of CAN Articles Per Year
Elaborate Schemes Explaining CAN At The
          Height of Its Popularity
Elaborate Schemes Explaining CAN At The
          Height of Its Popularity
In the early post-transplant biopsy, many specific
lesions which provide evidence of clinically
significant processes. Biopsy is helpful.
   Tubulitis – Rejection
   Intimal arteritis – Rejection
   Transmural arteritis – Rejection
   Hyaline arteriolar change – Calcineurin inhibitor toxicity
   Glomerulitis, peritubular capillary cell accumulation, C4d
    positivity – Antibody-mediated rejection
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In the late post-transplant biopsy, many non-
specific lesions. Often biopsy is not helpful.
   Interstitial fibrosis, tubular atrophy – Non-specific.
   Fibrous intimal thickening – Non-specific
   Chronic transplant glomerulopathy – Antibody-mediated
    rejection, or thrombotic microangiopathy or MPGN
    (hepatitis related)
   True chronic rejection vascular changes, with intimal
    arteritis, elastica breaks etc. – rare.
   Peritubular capillary multilayering on electron
    microscopy – usually chronic antibody mediated
    rejection.
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Sclerosing Rejection:
                   “neo-media” formation supe
                    imposed on donor disease
                      (0.9 years post grafting)




PAS stain




            Elastic stain
Transplant Glomerulitis and Glomerulopathy
       4.5 years post transplantation
Slide
 23
INTERSTITIAL FIBROSIS AND TUBULAR ATROPHY (IFTA)
IN RENAL ALLOGRAFTS
IFTA WITH INFLAMMATION – MENGEL ET AL.
INFILTRATES IN AREAS OF FIBROSIS AND TUBULAR ATROPHY
perivascular
SUBCAPSULAR
NODULAR INFILTRATES
BANFF I- AND TOTAL I-SCORE AND DIAGNOSIS: INTERSTITIAL INFILTRATES ARE
                           NOT DISEASE SPECIFIC

                                    *                    i-score        total i-score

                                                              *p<0.05

                                                                                        *

                                                  *
% cortex with infiltrate




                                                                                            *
                                                                   *


                                                         *
INFILTRATES IN BIOPSIES FOR CAUSE ARE TIME
DEPENDENT

                      100
                                     fibrosis/atrophy
                      90             i-Banff
                                     i-IFTA
                      80

                      70
  % cortex involved




                      60

                      50

                      40

                      30


                      20

                      10


                       0
                            1   6    11 16     21 26    31 36    41 46 51   56 61   66 71   76 81 86   91 96 101 106 111 116 121 126
                                      3                           8                  27                     79                246
                                    months                      months              months                 months            months
                                                                129 biopsies ordered by time post TX


                                                                                    Mengel et al. Am J Transplant. 2009 Jan;9(1):169-78.
Coming Full Circle – In the Original Banff Paper
                            .
The Editor Insisted We Put Everything About the
Non-Specificity of Interstitial Infiltrates at the
Beginning “So The Message Will Reach Even
Those Who Only Read The First Page!”
   Solez, K., Axelsen, R.A., Benediktsson, H., Burdick, J.F.,
    Cohen, A.H., Colvin, R.B.,Croker, B.P., Droz, D., Dunnill,
    M.S., Halloran, P.F., Hayry, P., Jennette, J.C., Keown, P.A.,
    Marcussen, N., Mihatsch, M.J., Morozumi, K., Myers, B.D.,
    Nast, C., Olsen, S., Racusen, L.C., Ramos, E.L., Rosen,
    S., Sachs, D.H., Salomon, D.R., Sanfilippo, F., Verani, R.,
    von Willebrand, E., and Yamaguchi, Y.: International
    standardization of nomenclature and criteria for the
    histologic diagnosis of renal allograft rejection : the Banff
    working classification of kidney transplant pathology.
    Kidney Int. 44:411-422, 1993.
CURRENT RESEARCH
 Microarray analysis of both human & mouse
  kidney transplants with rejection and other
  complications
 Correlate with Clinical data & Banff lesions.
  Common entities like glomerulonephritis,
  bacterial infection, and calcineurin inhibitor
  toxicity have no genomics signature at present.
Human and Mouse
similar genes and similar development




                                        The Cell 2002.
TABLE 1: CORRELATIONS BETWEEN INFILTRATE TYPES
AND PATHOGENESIS BASED TRANSCRIPT SETS (PBTS)



   Gene sets*#                                         i-Banff     t-score   i-IFTA   IFTA     nodular   perivascular

   T-cell associated (CATs)                                0.534   0.484     0.284    0.246     0.298        ns
   γ-Interferon dependent (GRITs)                          0.532   0.441     0.258    0.211     0.241        ns
   Kidney parenchyma associated (KTs)                  -0.296      -0.303    -0.199   -0.156     ns          ns

   Injury and repair associated (IRITs)                    0.379   0.355     0.246    0.206      ns          ns

   Immunoglobulin associated (IGTs)                        0.174     ns      0.434    0.398     0.336        ns

   B-cell associated (BATs)                                0.281   0.279     0.423    0.387     0.355        ns

  # given is the highest r-value revealed for one PBT of
            each particular biological process
              *Spearman correlation, p<0.001
Paula Blanco – Superiority of Virtual Microscopy




A                                                  B




C                                                  D
Figure 2.

    Average intra-observer reproducibility of 3 observers




                                                            0.90
                                                                                                                          all comparisons p>0.05
                                                            0.80
                                                            0.70
                    (overall kappa values)




                                                            0.60
                                                            0.50                                                                                                                     Virtual Slide
                                                            0.40                                                                                                                     Glass Slide

                                                            0.30
                                                            0.20
                                                            0.10
                                                            0.00
                                                                       g       i       t       v         ptc        cg        ci        ct        cv        ah        mm Diagnosis
                                                                                           v




                                                                                                                                                       ah
                                                                                                                                             cv
                                                                                   t




                                                                                                               cg
                                                                                                     c




                                                                                                                                   ct




                                                                                                                                                                  m
                                                                           i




                                                                                                                                                                             sis
                                                                   g




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                                                                                                   pt




                                                                                                                                                                 m

                                                                                                                                                                        no
                                                                                                                                                                         g
                                                                                                                                                                      ia
                                                                                                                                                                  D
Figure 3.
    Inter-observer reproducibility among 3 observers




                                                       0.90                                               p=0.04

                                                       0.80
                                                       0.70   p=0.03
                  (overall kappa values)




                                                                                        p=0.08
                                                       0.60
                                                                                                 p=0.03
                                                       0.50                                                                                    p=0.08                        Virtual Slide
                                                                       p=0.08                                               p=0.05
                                                                                   NS                                                                               p=0.08   Glass Slide
                                                       0.40                                                        p=0.03                                   NS

                                                       0.30                                                                          NS

                                                       0.20
                                                       0.10
                                                       0.00
                                                                  g        i       t        v     ptc      cg        ci        ct        cv        ah       mm Diagnosis
                                                                               t




                                                                                                                ci
                                                                                        v




                                                                                                     cg




                                                                                                                                              ah
                                                                       i




                                                                                                                          ct




                                                                                                                                                     m
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                                                                                                                                                                 is
                                                                                            pt




                                                                                                                                                                s
                                                                                                                                                    m

                                                                                                                                                           g no
                                                                                                                                                        ia
                                                                                                                                                        D
Figure 4.




                                                             p = 0.29
                                                                                           p = 0.11
            A.                                                                                                             B.
                                 100%                                                                                       100%
                                          Virtual vs. Virtual slides
Agreement rate in diagnosis




                                 90%                                                                                        90%
                                                                       Glass vs. Glass slides
                                 80%                                                                                        80%
                                                                                                Virtual vs. Glass slides
                                 70%                                                                                        70%

                                 60%                                                                                        60%                                   Virtual vs. Virtual slides
                                 50%                                                                                        50%                                   Glass vs. Glass slides

                                 40%                                                                                        40%                                   Virtual vs. Glass slides

                                 30%                                                                                        30%

                                 20%                                                                                        20%

                                 10%                                                                                        10%

                                  0%                                                                                            0%
                                                                                                                                     Observer 1 Observer 2 Observer 3
CHANGES NOT CONSIDERED TO BE DUE TO REJECTION:

   Post-transplant lymphoproliferative disorder




                                                                                                     Slide 39
   Non-specific changes
          a)   Focal interstitial inflammation without tubulitis: Nodular infiltrates, parivasular
               infiltrates.
          b)   Vascular changes: endothelial reactive changes, vacuolization, venulitis.

   Acute tubular injury
   Acute Interstitial nephritis
   Cyclosporine-associated changes, acute or chronic
   Subcapsular injury
   Pre-transplant acute endothelial injury
   Papillary necrosis
   De novo glomerulonephritis
   Recurrent disease
   Pre-existing disease
   Other-viral infection (CMV), obstruction and reflux
Slide 40
POST-TRANSPLANT LYMPHOPROLIFERATIVE
DISEASE (PTLD): WHO 2008
Early lesions
a. plasmacytic hyperplasia,

b. infectious mononucleosis type

Polymorphic PTLD
Monomorphic PTLD
a. B-cell neoplasms

b. T-cell neoplasms

Classic Hodgkin lymphoma-type PTLD
DIFFERENTIAL DIAGNOSIS OF PTLD
 T-cell rich PTLDs occur in 10-30% of cases
 EBV negative PTLDs occur in 10-30% of cases

 Endarteritis may be PTLD associated.

 PTLD is not associated with edema.
MY PRESENTATION TOMORROW “BANFF AND BEYOND”
CONTINUES THIS DISCUSSION, SO STAY TUNED!
 The pathologic spectrum of chronic allograft injury
  is very broad, and we should keep all entities in
  mind, even the rare ones. Technology is advancing
  in some areas much more quickly than you think,
  and in other areas not at all.
 Further conclusions (big and small!) tomorrow.

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Kim Solez Chronic Rejection

  • 1. Chronic rejection- current concepts and newer perspectives Kim Solez, M.D.
  • 2. Mentor influences: Smelling the Flowers Meetings – Not A Waste of Time!  “You should take time to smell the flowers.” (1972)  “Medical meetings are just social events. Nothing important happens at them. They are a waste of time. You should avoid organizing medical meetings.” - Robert H. Heptinstall, M.D.  I did not follow the latter advice. Physicians need to be socialized, humanized. Organized my first Acute Renal Failure Symposium in 1982, published as a book in 1984 Acute Renal Failure: Correlations Between Morphology and Function. Many other meetings since then. Banff meetings began 1991, continued every two years since then.  Technology and Future of Medicine course began 2011, mixes science and humanities, technological Singularity, futurism, exponential change.  High impact education changes human behavior, like advertising does. In the area of late biopsies and the scarred allograft in Banff consensus process we have been working to change behavior for some time.  Evolution of thinking from chronic rejection, to chronic allograft nephropathy, to interstitial fibrosis and tubular atrophy.
  • 3. An Evolution in Which We Find Evidence of the Human Tendency to Try to Believe in Specific Entities There Is No Evidence For!  Originally all late scarring processes in the transplanted kidney were called “chronic rejection”.  In order to stop perpetuating the idea that everything was chronic rejection we coined the term “chronic allograft pathology” – “CAN” for these nonspecific chronic changes.  People seized on CAN as a new entity, devised strategies to prevent it, animal models for it etc. Soon there were hundreds of articles about CAN.  To stop this artificial glorification of nonspecific changes as a new entity we eliminated the phrase CAN and used the descriptive terms interstitial fibrosis and tubular atrophy instead - IFTA.
  • 4. Number of CAN Articles Per Year
  • 5. Elaborate Schemes Explaining CAN At The Height of Its Popularity
  • 6. Elaborate Schemes Explaining CAN At The Height of Its Popularity
  • 7. In the early post-transplant biopsy, many specific lesions which provide evidence of clinically significant processes. Biopsy is helpful.  Tubulitis – Rejection  Intimal arteritis – Rejection  Transmural arteritis – Rejection  Hyaline arteriolar change – Calcineurin inhibitor toxicity  Glomerulitis, peritubular capillary cell accumulation, C4d positivity – Antibody-mediated rejection
  • 16. In the late post-transplant biopsy, many non- specific lesions. Often biopsy is not helpful.  Interstitial fibrosis, tubular atrophy – Non-specific.  Fibrous intimal thickening – Non-specific  Chronic transplant glomerulopathy – Antibody-mediated rejection, or thrombotic microangiopathy or MPGN (hepatitis related)  True chronic rejection vascular changes, with intimal arteritis, elastica breaks etc. – rare.  Peritubular capillary multilayering on electron microscopy – usually chronic antibody mediated rejection.
  • 19.
  • 20. Sclerosing Rejection: “neo-media” formation supe imposed on donor disease (0.9 years post grafting) PAS stain Elastic stain
  • 21.
  • 22. Transplant Glomerulitis and Glomerulopathy 4.5 years post transplantation
  • 24. INTERSTITIAL FIBROSIS AND TUBULAR ATROPHY (IFTA) IN RENAL ALLOGRAFTS
  • 25. IFTA WITH INFLAMMATION – MENGEL ET AL.
  • 26. INFILTRATES IN AREAS OF FIBROSIS AND TUBULAR ATROPHY
  • 29. BANFF I- AND TOTAL I-SCORE AND DIAGNOSIS: INTERSTITIAL INFILTRATES ARE NOT DISEASE SPECIFIC * i-score total i-score *p<0.05 * * % cortex with infiltrate * * *
  • 30. INFILTRATES IN BIOPSIES FOR CAUSE ARE TIME DEPENDENT 100 fibrosis/atrophy 90 i-Banff i-IFTA 80 70 % cortex involved 60 50 40 30 20 10 0 1 6 11 16 21 26 31 36 41 46 51 56 61 66 71 76 81 86 91 96 101 106 111 116 121 126 3 8 27 79 246 months months months months months 129 biopsies ordered by time post TX Mengel et al. Am J Transplant. 2009 Jan;9(1):169-78.
  • 31. Coming Full Circle – In the Original Banff Paper . The Editor Insisted We Put Everything About the Non-Specificity of Interstitial Infiltrates at the Beginning “So The Message Will Reach Even Those Who Only Read The First Page!”  Solez, K., Axelsen, R.A., Benediktsson, H., Burdick, J.F., Cohen, A.H., Colvin, R.B.,Croker, B.P., Droz, D., Dunnill, M.S., Halloran, P.F., Hayry, P., Jennette, J.C., Keown, P.A., Marcussen, N., Mihatsch, M.J., Morozumi, K., Myers, B.D., Nast, C., Olsen, S., Racusen, L.C., Ramos, E.L., Rosen, S., Sachs, D.H., Salomon, D.R., Sanfilippo, F., Verani, R., von Willebrand, E., and Yamaguchi, Y.: International standardization of nomenclature and criteria for the histologic diagnosis of renal allograft rejection : the Banff working classification of kidney transplant pathology. Kidney Int. 44:411-422, 1993.
  • 32. CURRENT RESEARCH  Microarray analysis of both human & mouse kidney transplants with rejection and other complications  Correlate with Clinical data & Banff lesions. Common entities like glomerulonephritis, bacterial infection, and calcineurin inhibitor toxicity have no genomics signature at present.
  • 33. Human and Mouse similar genes and similar development The Cell 2002.
  • 34. TABLE 1: CORRELATIONS BETWEEN INFILTRATE TYPES AND PATHOGENESIS BASED TRANSCRIPT SETS (PBTS) Gene sets*# i-Banff t-score i-IFTA IFTA nodular perivascular T-cell associated (CATs) 0.534 0.484 0.284 0.246 0.298 ns γ-Interferon dependent (GRITs) 0.532 0.441 0.258 0.211 0.241 ns Kidney parenchyma associated (KTs) -0.296 -0.303 -0.199 -0.156 ns ns Injury and repair associated (IRITs) 0.379 0.355 0.246 0.206 ns ns Immunoglobulin associated (IGTs) 0.174 ns 0.434 0.398 0.336 ns B-cell associated (BATs) 0.281 0.279 0.423 0.387 0.355 ns # given is the highest r-value revealed for one PBT of each particular biological process *Spearman correlation, p<0.001
  • 35. Paula Blanco – Superiority of Virtual Microscopy A B C D
  • 36. Figure 2. Average intra-observer reproducibility of 3 observers 0.90 all comparisons p>0.05 0.80 0.70 (overall kappa values) 0.60 0.50 Virtual Slide 0.40 Glass Slide 0.30 0.20 0.10 0.00 g i t v ptc cg ci ct cv ah mm Diagnosis v ah cv t cg c ct m i sis g ci pt m no g ia D
  • 37. Figure 3. Inter-observer reproducibility among 3 observers 0.90 p=0.04 0.80 0.70 p=0.03 (overall kappa values) p=0.08 0.60 p=0.03 0.50 p=0.08 Virtual Slide p=0.08 p=0.05 NS p=0.08 Glass Slide 0.40 p=0.03 NS 0.30 NS 0.20 0.10 0.00 g i t v ptc cg ci ct cv ah mm Diagnosis t ci v cg ah i ct m g c cv is pt s m g no ia D
  • 38. Figure 4. p = 0.29 p = 0.11 A. B. 100% 100% Virtual vs. Virtual slides Agreement rate in diagnosis 90% 90% Glass vs. Glass slides 80% 80% Virtual vs. Glass slides 70% 70% 60% 60% Virtual vs. Virtual slides 50% 50% Glass vs. Glass slides 40% 40% Virtual vs. Glass slides 30% 30% 20% 20% 10% 10% 0% 0% Observer 1 Observer 2 Observer 3
  • 39. CHANGES NOT CONSIDERED TO BE DUE TO REJECTION:  Post-transplant lymphoproliferative disorder Slide 39  Non-specific changes a) Focal interstitial inflammation without tubulitis: Nodular infiltrates, parivasular infiltrates. b) Vascular changes: endothelial reactive changes, vacuolization, venulitis.  Acute tubular injury  Acute Interstitial nephritis  Cyclosporine-associated changes, acute or chronic  Subcapsular injury  Pre-transplant acute endothelial injury  Papillary necrosis  De novo glomerulonephritis  Recurrent disease  Pre-existing disease  Other-viral infection (CMV), obstruction and reflux
  • 41. POST-TRANSPLANT LYMPHOPROLIFERATIVE DISEASE (PTLD): WHO 2008 Early lesions a. plasmacytic hyperplasia, b. infectious mononucleosis type Polymorphic PTLD Monomorphic PTLD a. B-cell neoplasms b. T-cell neoplasms Classic Hodgkin lymphoma-type PTLD
  • 42. DIFFERENTIAL DIAGNOSIS OF PTLD  T-cell rich PTLDs occur in 10-30% of cases  EBV negative PTLDs occur in 10-30% of cases  Endarteritis may be PTLD associated.  PTLD is not associated with edema.
  • 43. MY PRESENTATION TOMORROW “BANFF AND BEYOND” CONTINUES THIS DISCUSSION, SO STAY TUNED!  The pathologic spectrum of chronic allograft injury is very broad, and we should keep all entities in mind, even the rare ones. Technology is advancing in some areas much more quickly than you think, and in other areas not at all.  Further conclusions (big and small!) tomorrow.