Isolated liner exchange in revision total hip arthroplasty for the treatment of polyethylene wear is an increasingly common surgical procedure. Twenty-four hips underwent this procedure via the direct lateral approach and were prospectively followed clinically and radiographically. Accessible osteolytic lesions were curetted and bone grafted. At a mean follow-up of forty months, a significant clinical improvement was observed. One cup collapsed into an osteolytic lesion postoperatively; all other lesions regressed. No dislocations have occurred. Isolated liner exchange via the direct lateral approach may reduce dislocation rates while avoiding the morbidity associated with the removal of well-fixed components.

The purpose of this study was to evaluate the clinical and radiographic results of isolated liner exchange in revision total hip arthroplasty (THA) for osteolysis and polyethylene wear via the direct lateral surgical approach.

Retention of well-fixed implants avoids unnecessary bone loss at revision surgery. Previous studies report a significant dislocation rate with isolated liner exchange. Revision via the direct lateral surgical approach may reduce the dislocation rate in surgery for acetabular osteolysis.

Twenty-four hips that underwent an isolated liner exchange revision procedure via the direct lateral approach were prospectively followed. Accessible osteolytic lesions were curetted and bone grafted. Harris Hip Score, WOMAC Index, and radiographic analysis were recorded. The area of osteolytic lesions was calculated using a computer imaging technique.

At mean follow-up of forty months, all except one of the osteolytic lesions had regressed in size. Mean Harris Hip scores improved from sixty-nine to eighty-three and WOMAC indices improved from thirty-seven to twenty-four. No dislocations have occurred. One cup collapsed into an osteolytic lesion postoperatively, requiring an acetabular revision procedure.

Isolated liner exchange is a promising technique that avoids the removal of well-fixed acetabular implants. The increased dislocation rate associated with revision THA may be reduced and osteolytic lesions may be debrided and bone grafted through the direct lateral approach.

Isolated liner exchange via the direct lateral approach reduces the dislocation rate in THA. Retention of wellfixed implants and bone grafting is a procedure that preserves bone stock and addresses osteolytic lesions at revision surgery.

Introduction and Aims: Polyethylene wear in total hip arthroplasty (THA) is frequently associated with wellfixed cementless implants. Purpose: To evaluate the clinical and radiographic results of the isolated liner exchange (ILE) procedure in revision THA via the direct lateral surgical approach.

Method: A prospective study of 24 hips that underwent an ILE revision procedure via the direct lateral approach was conducted. Accessible osteolytic lesions were managed with curettage and bone grafting. Clinical data including Harris hip score, WOMAC Index, SF-12, and radiographic analysis were recorded. The area of osteolytic lesions was calculated using a new software program.

Results: This is the first study to our knowledge to report on the results of the ILE procedure performed via the direct lateral surgical exposure. Twenty-three patients underwent 24 revisions with an ILE. At mean follow-up of 40 months, all osteolytic lesions had regressed. Harris hip scores improved from 69 to 83. WOMAC indices improved from 37 to 24. No dislocations have occurred. Two patients have required revision. Isolated liner exchange for polyethylene wear is a promising technique that avoids the removal of well-fixed acetabular implants. The increased dislocation rate associated with this revision THA procedure may be reduced and osteolytic lesions may be successfully debrided and bone grafted through the direct lateral approach.

Conclusion: The ILE procedure, when performed via the direct lateral surgical approach, may reduce the dislocation rate commonly reported via the posterolateral exposure with this procedure. Retention of well-fixed implants and bone grafting preserves bone stock and adequately addresses osteolytic lesions at revision surgery through this exposure.

This paper presents radiological changes in femoral cortical allograft used to replace the disc in low back and leg pain syndromes. The technique originated with the use of patient’s own iliac crest but donor site pain and lack of rotational control with removal of the annulus resulted in a) femoral cortical allograft supplemented with b) posterior fixation, more recently of the trans-laminar screw variety.

Experience with over 200 patients with femoral cortical allograft indicated that the rejection rate is virtually nil. Early changes include the loss of line between donor and host bone as early as three to four weeks after surgery.

There is radiological evidence in some cases that radiological healing has taken place by four weeks. There is no radiological difference whether the patient’s own bone or allograft chips are used to pack the allograft cavity. At one year and beyond, the gap behind the allograft in the interbody space fills with host bone, thus avoiding any posterior migration of the allograft plug. There is some subsidence, over the first 12 months, into host bone. Attention to detail in surgical treatment of the end-plate is an important part of the technique.

Axial views show dramatic changes up to 10 years after surgery. Gradual erosion of allograft by host bone, both at the external and internal diameter, occurs. Finally, there is the merest shell of donor bone identified, the rest clearly replaced by host bone. Unfortunately, biopsy samples to corelate with the radiological films are not available.

Allograft bone in surgery was original with MacEwen of Glasgow (1880). Its use 30 years ago in scoliosis surgery was generally not successful. The interbody femoral cortical allograft succeeds by reason of the surgical principles involved: 1) Thorough clearance of all avascular (disc) tissue – thus, the provision of a thoroughly vascularised bed; 2) Rigid fixation (provided by the translaminar screw fixation). For reasons of cost, mechanics, biological behaviour and ease of shaping before insertion, femoral cortical allograft has provided an excellent long-term disc replacement.

Purpose and Background: We have previously reported our investigations of nerve ingrowth into intervertebral discs (IVD) from patients with mechanical low back pain. We have shown that in discs that are painful on discography (pain level discs) nerves actively grow into the deep annulus fibrosus and nucleus pulposus. Nerve ingrowth accompanies blood vessel ingrowth and advances into the nucleus pulposus from the end plate. The morphology and neurochemistry of these nerves indicate them to be nociceptive.

The growth of non-myelinated pain fibres in other settings is regulated by the cytokine Nerve Growth Factor (NGF). In this study, we have investigated the production and distribution of NGF, or more particularly its active isoform – NGF-β, and its receptors, in diseased intervertebral discs in order to establish whether this cytokine might be responsible for the observed nerve ingrowth in this situation.

Methods: Tissue sections of 21 pain level, 15 non-pain level diseased and 12 normal intervertebral discs, taken at the time of spinal surgery, and from cadavers, were probed by radioactive in situ hybridisation (ISH) for expression of NGF-β, and by immunohistochemistry (IHC) for its high and low affinity receptors (trk-A and p75 respectively). In addition, either serial sections were stained with cell specific markers (CD31 – endothelial cell, PGP9.5 – neurones, GAP43 – actively growing nerves) or sections were doubled stained (two antibodies or both ISH and IHC).

Results: We have demonstrated that NGF-β is synthesised by the endothelial cells of blood vessels growing into the IVD from the end plate. The high affinity receptor is expressed by those small nerve fibres that accompany the vessels and in their offshoots in pain level discs that are growing from perivascular nerves into the disc. In addition to their expressing the nerve specific molecule PGP9.5, the trk-A positive cells also express the nerve growth associated protein GAP43.

Conclusion: The data indicate that nerve ingrowth into IVD is regulated by NGF-β. We have localised this production to the endothelial cells of ingrowing blood vessels. NGF-β is a potential therapeutic target for the management of back pain.

Purpose and Background: There is increasing evidence that events within the diseased intervertebral disc (IVD) are mediated by locally synthesised cytokines. A prominent histological, imaging and surgical feature of IVD disease is degradation of the cartilaginous discal matrix. Whilst the mechanism by which this is mediated is unknown, in other situations where connective tissues are degraded degradation is the result of production of matrix-degrading enzymes by local connective tissue cells stimulated by cytokines, particularly the beta isoform of interleukin-1 (IL-1β). Included amongst these disorders is osteoarthritis (OA) of diarthrodial joints. OA has many similarities to the discal “degeneration” seen in mechanical back pain syndromes. In the current study, we have used a combination of in-situ techniques to establish if IL-1β is responsible for stimulating matrix degradation in the IVD.

Methods: Using a combination of radioactive in-situ hybridisation (ISH) and competitive in situ zymography (ISZ) we have studied expression of IL-1β and IL-1R – its type 1 receptor (ISH) and matrix degradation (ISZ) in five diseased lumbar IVD taken at spinal fusion surgery and 10 cadaveric IVD (five normal and five diseased). The nucleus pulposus (NP) was separated from the annulus fibrosus and diced into 0.5cm cubes. Half the cubes (typically three) were fixed in formalin and processed into paraffin wax for ISH, and half were used for ISZ. For ISH, 5 μm sections of paraffin-embedded tissue were reacted with cDNA probes radiolabelled with 35S to 580 and 530 base segments of the IL-1β and IL-1R molecules. Hybridisation was disclosed using autoradiography. For ISZ, 50 μm vibratome sections were placed into wells on microscope slides precoated with gelatin. Sections were incubated for 10 days, half in culture medium and half in medium supplemented with human recombinant IL-1 receptor antagonist (IL-1Ra – an inhibitor of IL-1). Sections were photographed at daily intervals to detect evidence of gel degradation.

Results: Chondrocytes within patient and cadaveric diseased but not normal discs expressed mRNA for both IL-1β and IL-1R. By ISZ, the same cells degraded gelatin. Degradation was inhibited by recombinant IL-1Ra.

Conclusion: This study shows that chondrocytes of diseased discs express IL-1 and its receptor. The same cells produced matrix-degrading enzymes by a mechanism that can be inhibited by the IL-1 inhibitor IL-1Ra. IL-1 is a potential therapeutic target for the management of IV disc disease.

We treated 22 patients with type-two odontoid fractures in halothoracic vests for six to eight weeks followed by a Philadelphia collar for four weeks. Eighteen patients were reviewed by questionnaire and radiography at a mean of 40 months after injury. We assessed union, fracture position, the degree of permanent pain and stiffness, satisfaction with the treatment and the outcome.

The overall union rate was 82%. Posterior malunion with residual posterior displacement or angulation was associated with a higher incidence of persisting pain. The position at union did not correlate with the residual cervical stiffness. Fractures failed to unite in four patients (18%) none of whom had late neurological sequelae, although they had more late pain. There were associations between the development of nonunion and an extension-type injury, age over 65 years and delay in diagnosis.