Acta Chir Orthop Traumatol Cech. 2015; 82(2):126-134 | DOI: 10.55095/achot2015/018

Přínos Morawietzovy klasifikace k hodnocení periprotetických tkáníPůvodní práce

J. GALLO1,*, P. LU®NÁ2, M. HOLINKA1, J. EHRMANN2, J. ZAPLETALOVÁ3, J. LO©«ÁK1
1 Ortopedická klinika LF UP a FN Olomouc
2 Ústav histologie a embryologie, LF UP v Olomouci
3 Ústav lékařské biofyziky, LF UP v Olomouci

PURPOSE OF THE STUDY:
A consensual classification of the periprosthetic interface membrane obtained at revision total joint arthroplasty was published by Morawietz et al. in 2006. Based on histomorphological criteria, four types of periprosthetic membrane were proposed: type I, aseptic failure; type II, septic failure; type III, combined type (carrying signs of both type I and II); and type IV, indeterminate type. The aim of this study was to find out whether and to what extent the Morawietz system would be suitable for use at an independent institution involved in the evaluation of periprosthetic membranes for a long time. Should it appear that the institution achieved an equally good or even better agreement between the clinical diagnosis and the histopathological finding, this consensus classification could be recommended for routine use.

MATERIAL AND METHODS:
The samples of periprosthetic tissue evaluated in this study were obtained during surgery from the following groups of patients: 66 patients with aseptic loosening of total hip (THA) or knee arthroplasty, 15 patients with infection of THA, 16 patients with THA without any signs of aseptic loosening, osteolysis or infection; 8 patients with hip osteoarthritis and 8 patients with knee osteoarthritis. Sample collection and processing (for purposes of histomorphological evaluation and immunohistochemical staining) was performed according to the established protocol. The tissue samples evaluation was made by an experienced pathologist hand in hand with the method described in the original paper by Morawietz et al. For a more detailed tissue analysis, selected antibodies (CD4, CD8, CD20, IFN-γ and Hsp-60) were visualized by immunohistochemistry.

RESULTS:
The majority of samples from aseptic reoperations were classified as membranes of the type I (79%) and III (16%). Specimens retrieved from septic cases were mostly classified as membranes of type II and III (60% together). The septic membranes showed a significantly higher expression of CD20 protein when compared with both the aseptic (p < 0.0001) and control THA samples (p = 0.003). The membranes retrieved from the surroundings of a stable THA without osteolysis and infection had lower expression levels of Hsp60 and IFN-γ, when compared with those from both aseptic and septic loosening. Finally, Hsp-60 expression was significantly higher in osteoarthritic tissue than in samples from stable THA (p = 0.041).

DISCUSSION:
Morawietz et al. proposed a standardized classification system for evaluation of periprosthetic tissue. As any attempt at generalization of a complex issue, this proposal has certain shortcomings. One of these is poor detection of chronic and low-grade infections. A method that would improve the conventional counting of polymorphonuclear leukocytes is still being sought. In this connection, immunostaining for CD20 combined with an assessment of antimicrobial peptides may be a promising option. The supplementary specimen staining showed that pseudosynovial tissue is much more active in patients carrying infection and the least active in samples from stable THA in which certain tolerance and thus tissue homeostasis might be expected.

CONCLUSIONS:
1. In this study the distribution of findings classified according to the Morawietz system was similar to the results published in the original study from 2006.
2. The definition of an aseptic membrane (type I) in the Morawietz system meets the requirements of clinical practice (agreement, about 80%).
3. An increased sensitivity for infectious membrane detection can be achieved by using supplementary immunohistochemical staining effective particularly in chronic and low-grade infections.
4. Painless and stable THAs typically have very low expression levels of CD4, CD20 and Hsp-60 proteins, and interferon-gamma (IFN-γ) as well.

Klíčová slova: total hip arthroplasty, total knee arthroplasty, aseptic loosening, prosthetic joint infection, tissue analysis, membranes, CD receptors, Hsp-60 protein, IFN-γ

Zveřejněno: 1. duben 2015  Zobrazit citaci

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GALLO J, LU®NÁ P, HOLINKA M, EHRMANN J, ZAPLETALOVÁ J, LO©«ÁK J. Přínos Morawietzovy klasifikace k hodnocení periprotetických tkání. Acta Chir Orthop Traumatol Cech. 2015;82(2):126-134. doi: 10.55095/achot2015/018. PubMed PMID: 26317183.
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    Reference

    1. BELLAYE, P. S., BURGY, O., CAUSSE, S., GARRIDO, C., BONNIAUD, P.: Heat shock proteins in fibrosis and wound healing: good or evil? Pharmacol. Ther., 143: 119-132, 2014. Přejít k původnímu zdroji... Přejít na PubMed...
    2. BORI, G., MUNOZ-MAHAMUD, E., GARCIA, S., MALLOFRE, C., GALLART, X., BOSCH, J., GARCIA, E., RIBA, J., MENSA, J., SORIANO, A.: Interface membrane is the best sample for histological study to diagnose prosthetic joint infection. Mod. Pathol., 24: 579-584, 2011. Přejít k původnímu zdroji... Přejít na PubMed...
    3. CIERNY, G., 3RD, MADER, J. T., PENNINCK, J. J.: A clinical staging system for adult osteomyelitis. Clin. Orthop. Relat. Res., 414: 7-24, 2003. Přejít k původnímu zdroji... Přejít na PubMed...
    4. DAPUNT, U., GIESE, T., PRIOR, B., GAIDA, M. M., HANSCH, G. M.: Infectious versus non-infectious loosening of implants: activation of T lymphocytes differentiates between the two entities. Int. Orthop., 38: 1291-1296, 2014. Přejít k původnímu zdroji... Přejít na PubMed...
    5. FUJISHIRO, T., MOOJEN, D. J., KOBAYASHI, N., DHERT, W. J., BAUER, T. W.: Perivascular and diffuse lymphocytic inflammation are not specific for failed metal-on-metal hip implants. Clin. Orthop. Relat. Res., 469: 1127-1133, 2011. Přejít k původnímu zdroji... Přejít na PubMed...
    6. FULÍN, P., POKORNÝ, D., ©LOUF M., VACKOVÁ, T., DYBAL, J., SOSNA, A.: [Effect of sterilisation with formaldehyde, gamma irradiation and ethylene oxide on the properties of polyethylene joint replacement components]. Acta Chir. orthop. Traum. čech., 81: 33-39, 2014. Přejít k původnímu zdroji...
    7. GALLO, J., KOLAR, M., DENDIS, M., LOVECKOVA, Y., SAUER, P., ZAPLETALOVA, J., KOUKALOVA, D.: Culture and PCR analysis of joint fluid in the diagnosis of prosthetic joint infection. New Microbiol., 31: 97-104, 2008.
    8. GALLO, J., VACULOVA, J., GOODMAN, S.B., KONTTINEN, Y.T., THYSSEN, J. P.: Contributions of human tissue analysis to understanding the mechanisms of loosening and osteolysis in total hip replacement. Acta Biomater., 10: 2354-2366, 2014. Přejít k původnímu zdroji... Přejít na PubMed...
    9. GREENFIELD, E. M., BI, Y., RAGAB, A. A., GOLDBERG, V. M., NALEPKA, J. L., SEABOLD, J. M..: Does endotoxin contribute to aseptic loosening of orthopedic implants? J. Biomed. Mater. Res. B. Appl. Biomater., 72: 179-185, 2005. Přejít k původnímu zdroji... Přejít na PubMed...
    10. IOANNIDIS, J. P.: Why most published research findings are false. PLoS Med., 2: e124, 2005. Přejít k původnímu zdroji... Přejít na PubMed...
    11. JANZ, V., WASSILEW, G.I., HASART, O., MATZIOLIS, G., TOHTZ, S., PERKA, C.: Evaluation of sonicate fluid cultures in comparison to histological analysis of the periprosthetic membrane for the detection of periprosthetic joint infection. Int. Orthop., 37: 931-936, 2013. Přejít k původnímu zdroji... Přejít na PubMed...
    12. KONTTINEN, Y. T., XU, J. W., WARIS, E., LI T. F., GOMEZ-BARRENA, E., NORDSLETTEN, L., SANTAVIRTA, S.: Interleukin-6 in aseptic loosening of total hip replacement prostheses. Clin. Exp. Rheumatol., 20: 485-490, 2002.
    13. KOULOUVARIS, P., LY, K., IVASHKIV, L. B., BOSTROM, M. P., NESTOR, B. J., SCULCO, T. P., PURDUE, P. E.: Expression profiling reveals alternative macrophage activation and impaired osteogenesis in periprosthetic osteolysis. J. Orthop. Res., 26:,106-116, 2008. Přejít k původnímu zdroji... Přejít na PubMed...
    14. KRENN, V., MORAWIETZ, L., KIENAPFEL, H., ASCHERL, R., MATZIOLIS, G., HASSENPFLUG, J., THOMSEN, M., THOMAS, P., HUBER, M., SCHUH, C., KENDOFF, D., BAUMHOER, D., KRUKEMEYER, M.G., PERINO, G., ZUSTIN, J., BERGER, I., RUTHER, W., POREMBA, C., GEHRKE, T.: [Revised consensus classification. Histopathological classification of diseases associated with joint endoprostheses]. Z. Rheumatol., 72: 383-392, 2013. Přejít k původnímu zdroji... Přejít na PubMed...
    15. LI, T. F., SANTAVIRTA, S., WARIS, V., LASSUS, J., LINDROOS, L., XU, J. W., VIRTANEN, I., KONTTINEN, Y. T.: No lymphokines in T-cells around loosened hip prostheses. Acta Orthop. Scand., 72: 241-247, 2001. Přejít k původnímu zdroji... Přejít na PubMed...
    16. MIRRA, J. M., AMSTUTZ, H. C., MATOS, M., GOLD, R.: The pathology of the joint tissues and its clinical relevance in prosthesis failure. Clin. Orthop. Relat. Res., 117: 221-240, 1976. Přejít k původnímu zdroji...
    17. MOOJEN, D. J., VAN HELLEMONDT, G., VOGELY, H. C., BURGER, B. J., WALENKAMP, G. H., TULP, N. J., SCHREURS, B. W., DE MEULEMEESTER, F. R., SCHOT, C. S., VAN DE POL, I., FUJISHIRO, T., SCHOULS, L. M., BAUER, T. W., DHERT, W. J.: Incidence of low-grade infection in aseptic loosening of total hip arthroplasty. Acta Orthop., 81: 667-673, 2010. Přejít k původnímu zdroji... Přejít na PubMed...
    18. MORAWIETZ, L., CLASSEN, R. A., SCHRODER, J. H., DYNYBIL, C., PERKA, C., SKWARA, A., NEIDEL, J., GEHRKE, T., FROMMELT, L., HANSEN, T., OTTO, M., BARDEN, B., AIGNER, T., STIEHL, P., SCHUBERT, T., MEYER-SCHOLTEN, C., KONIG, A., STROBEL, P., RADER, C.P., KIRSCHNER, S., LINTNER, F., RUTHER, W., BOS, I., HENDRICH, C., KRIEGSMANN, J., KRENN, V.: Proposal for a histopathological consensus classification of the periprosthetic interface membrane. J. Clin. Pathol., 59: 591-597, 2006. Přejít k původnímu zdroji... Přejít na PubMed...
    19. MORAWIETZ, L., TIDDENS, O., MUELLER, M., TOHTZ, S., GANSUKH, T., SCHROEDER, J. H., PERKA, C., KRENN, V.: Twenty-three neutrophil granulocytes in 10 high-power fields is the best histopathological threshold to differentiate between aseptic and septic endoprosthesis loosening. Histopathology, 54: 847-853, 2009. Přejít k původnímu zdroji... Přejít na PubMed...
    20. NYGAARD, M., BASTHOLM, L., ELLING, F., SOBALLE, K., BORGWARDT, A.: Can ultrastructural particle location predict aseptic loosening? A biopsy study of nonloose hip implants one year postoperative using three bearing material combinations. J. Long Term Eff. Med. Implants., 17: 321-334, 2007. Přejít k původnímu zdroji... Přejít na PubMed...
    21. PANDEY, R., DRAKOULAKIS, E., ATHANASOU, N. A.: An assessment of the histological criteria used to diagnose infection in hip revision arthroplasty tissues. J. Clin. Pathol., 52: 118-123, 1999. Přejít k původnímu zdroji... Přejít na PubMed...
    22. RAUCH, I., MULLER, M., DECKER, T.: The regulation of inflammation by interferons and their STATs. JAKSTAT, 2: e23820, 2013. Přejít k původnímu zdroji... Přejít na PubMed...
    23. SHANBHAG, A. S., KAUFMAN, A. M., HAYATA, K., RUBASH, H. E.: Assessing osteolysis with use of high-throughput protein chips. J. Bone Jt Surg., 89-A: 1081-1089, 2007. Přejít k původnímu zdroji... Přejít na PubMed...
    24. SIERRA, J. M., GARCIA, S., MARTINEZ-PASTOR, J. C., TOMAS, X., GALLART, X., VILA, J., BORI, G., MACULE, F., MENSA, J., RIBA, J., SORIANO, A.: Relationship between the degree of osteolysis and cultures obtained by sonication of the prostheses in patients with aseptic loosening of a hip or knee arthroplasty. Arch. Orthop. Trauma Surg., 131: 1357-1361, 2011. Přejít k původnímu zdroji... Přejít na PubMed...
    25. TAKACOVA, S., SLANY, R., BARTKOVA, J., STRANECKY, V., DOLEZEL, P., LUZNA, P., BARTEK, J., DIVOKY, V.: DNA damage response and inflammatory signaling limit the MLL-ENL-induced leukemogenesis in vivo. Cancer Cell., 21: 517-531, 2012. Přejít k původnímu zdroji... Přejít na PubMed...
    26. THOMAS, P., IGLHAUT, G., WOLLENBERG, A., CADOSCH, D., SUMMER, B.: Allergy or tolerance: reduced inflammatory cytokine response and concomitant IL-10 production of lymphocytes and monocytes in symptom-free titanium dental implant patients. Biomed. Res. Int., 2013: 539834, 2013. Přejít k původnímu zdroji... Přejít na PubMed...
    27. TSARAS, G., MADUKA-EZEH, A., INWARDS, C. Y., MABRY, T., ERWIN, P. J., MURAD, M. H., MONTORI, V. M., WEST, C. P., OSMON, D. R., BERBARI, E. F.: Utility of intraoperative frozen section histopathology in the diagnosis of periprosthetic joint infection: a systematic review and meta-analysis. J. Bone Jt Surg., 94-A: 1700-1711, 2012. Přejít k původnímu zdroji... Přejít na PubMed...

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