IS THERE A GENETIC PREDISPOSITION TO ALVAL?

Langton D, Sidaginamale R, Wells S, et al. IS THERE A GENETIC PREDISPOSITION TO ALVAL?. Orthop Procs. 2019;101-B(SUPP_6):25-25. doi:10.1302/1358-992X.2019.6.025

Langton, D, et al. “IS THERE A GENETIC PREDISPOSITION TO ALVAL?.” Orthopaedic Proceedings, vol. 101-B, no. SUPP_6, 2019, pp. 25-25., https://doi.org/10.1302/1358-992X.2019.6.025

Langton, D., Sidaginamale, R., Wells, S., Wainwright, B., Holland, J., Deehan, D., Joyce, T., Jafri, A., Nargol, A., & Natu, S. (2019). IS THERE A GENETIC PREDISPOSITION TO ALVAL?. Orthopaedic Proceedings, 101-B(SUPP_6), 25-25. https://doi.org/10.1302/1358-992X.2019.6.025

Langton, D., Sidaginamale, R., Wells, S., Wainwright, B., Holland, J., Deehan, D. et al. (2019) “IS THERE A GENETIC PREDISPOSITION TO ALVAL?.” Orthopaedic Proceedings, 101-B(SUPP_6), pp. 25-25. Available at: https://doi.org/10.1302/1358-992X.2019.6.025

Langton, D, R Sidaginamale, S Wells, B Wainwright, J Holland, D Deehan, T Joyce, A Jafri, A Nargol, and S Natu. “IS THERE A GENETIC PREDISPOSITION TO ALVAL?.” Orthopaedic Proceedings 101-B, no. SUPP_6 (2019): 25-25. https://doi.org/10.1302/1358-992X.2019.6.025

Langton D, Sidaginamale R, Wells S, Wainwright B, Holland J, Deehan D, et al. IS THERE A GENETIC PREDISPOSITION TO ALVAL?. Orthop Procs. 2019 May 1;101-B(SUPP_6):25-25. https://doi.org/10.1302/1358-992X.2019.6.025

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Abstract

Introduction

We aimed to identify genes associated with the development of ALVAL at relatively low levels of wear.

Methods

At our unit all patients undergoing revision of a MoM hip prosthesis have periprosthetic tissue samples graded for ALVAL. Explants undergo volumetric wear testing of the bearing and taper surfaces. We identified patients with moderate/severe ALVAL who had been exposed to lower than the median wear rate of all recorded patients who had developed ALVAL (<3mm³/year). This was termed the “ALVAL” group. We then identified all patients whose tissues had shown no signs of ALVAL. The patients in the two groups were sent buccal DNA collection kits. DNA was examined using next generation sequencing. Alleleic frequencies in the two groups were compared using Fisher's test and compared to a background UK population group (n=8514). We then conducted binary logistic regression with patient age, sex, primary source of debris (taper/bearing) and HLA genotype as the predictors. With the hypothesis that a cobalt/albumin metalloprotein acts as the epitope, we used validated binding prediction software to determine the relative affinities of the binding grooves created by different DQA1/DQB1 genetic combinations for albumin derived peptides. Given the protection that male sex and younger age appears to confer against ALVAL, we hypothesized that testosterone peptides may compete for these binding sites.

Results

28 ALVAL and 37 non ALVAL patients returned their samples for testing. The frequencies of DQA1∗05:05 and DQB1∗03:01 were significantly greater in the ALVAL groups(p=0.018). The variables positively associated with ALVAL were female sex(0.021), increasing age(0.003) and DQA1/DQB1 combinations with greater binding affinity for albumin fragments(0.03). Greater binding affinities for testosterone peptides were inversely related to ALVAL(0.05).

Discussion

Common immune genotypes are associated with a greater risk of ALVAL.

Conclusion

The evidence base on which MoM follow up protocols are based should be re-evaluated in light of these findings and future studies designed accordingly.

Email: djlangton22@doctors.org.uk