A 65-year-old man presented in February 2007 with deteriorating renal function, creatinine 208 μmol/L (reference range 60-120 μmol/L). His background included chronic obstructive pulmonary disease and radiologically diagnosed asbestosis, previous duodenitis and pericarditis in 1970. His regular medications included a statin, a proton pump inhibitor, aspirin and an antimuscarinic bronchodilator. His urinalysis showed protein 1+, blood 4+ and his serum immunology showed a positive pANCA and myeloperoxidase (MPO) antibody. His C-reactive protein (CRP) was 33 mg/L. He underwent renal biopsy which showed evidence of an inactive vasculitis; 25 glomeruli (11 normal, 7 sclerosed, 7 showing fibrous crescents, 0 showing cellular crescents). There was patchy tubular atrophy, focal secondary interstitial inflammation and fibrosis. Immunofluoresence was negative. Silver stain was unremarkable. This was all in keeping with a pANCA-associated renal vasculitis that was currently quiescent. He maintained a stable creatinine with CRP <8 mg/L and was managed conservatively with close monitoring. In November 2007 it was noted he had a rising creatinine reaching 309 μmol/L prompting the initiation of prednisolone 80 mg and cyclophosphamide 200 mg with co-trimoxazole prophylaxis. His creatinine fell to 146 μmol/L by April 2008 with this regimen and his prednisolone was slowly weaned. Cyclophosphamide was discontinued due to leucopaenia seven weeks after commencement and this was replaced with azathioprine 150 mg. In July 2008 he had lower respiratory tract symptoms with raised inflammatory markers and was suspected of having active pulmonary involvement of his vasculitis. He underwent high resolution CT scanning of the chest which demonstrated areas of sub-pleural reticular shadowing, many related to areas of pleural thickening. He was noted to have a marked reduction in gas transfer (to 30% predicted), as well as a restrictive defect on spirometry. His azathioprine was changed to mycophenolate mofetil (MMF) 1 g bd as his CRP remained elevated (at 24 mg/L) with continued clinical vasculitic activity. By September 2008 his creatinine rose to 198 μmol/L with continued pANCA positivity and his CRP was elevated at 60 mg/L. In view of cyclophosphamide induced leucopaenia and failure of control with MMF, he was commenced on Rituximab 375 mg/m2 weekly for four weeks. At this stage his prednisolone dose was 25 mg. In November 2008 he presented to his general practitioner with a three-week history of progressive weakness of the left leg and sensory loss up to T10 dermatome level followed by urinary and faecal retention. He complained of buttock pain and also some similar right-sided symptoms, which was consistent with a clinical diagnosis of transverse myelitis. There was no optic involvement. He was referred to the Spinal team who requested an MRI demonstrating patchy, slightly nodular central enhancement at T10 extending to the conus. MRI head was normal. The radiological differential diagnosis included a primary cord neoplasm such as astrocytoma or less likely ependymoma. He was referred to the Neurologists and underwent CT scanning of the chest, abdomen and pelvis. This confirmed no primary malignancy or evidence of metastatic disease. He underwent CSF examination showing 10 × 106/l lymphocytes with no malignant cells, protein of 0.9 g/L. An antibody to aquaporin-4 was negative, as was lupus and antiphospholipid serology. He was referred for biopsy of the cord lesion. However, he had a boost in his dose of steroids and it was suggested to repeat the MRI scan before cord biopsy. The repeat MRI showed that the large lesion involving the lower thoracic cord had now almost completely resolved and the area of enhancement seen in the lower cord was no longer present. There was a new lesion extending from C7 down to T3. This was similar to the original lesion in that it was expansile and returned high signal on T2 weighted images with a much smaller area of central ring enhancement. It was felt that these changes made malignancy seem extremely unlikely as the affected areas had changed with time and increased immunosuppression. Vasculitis was suggested as a unifying diagnosis for his symptoms, the increase in steroids explaining the drastic MRI changes. His CRP peaked at 137 mg/L and dropped to 7 mg/L. Hence cord biopsy was not undertaken and his steroids continued at high dose, MMF stopped and rituximab continued. He was discharged and a further outpatient MRI showed continued improvement and his steroids were weaned down. In May 2009 he returned to hospital following further left sided pain. He was treated for a vasculitis flare. He underwent repeat MRI head and spine. This showed a single high focus in the right cerebellar hemisphere. He was treated with intravenous methylprednisolone and further rituximab treatment was arranged. His last dose of rituximab was December 2009. In February 2010 he was again admitted with left sided pain and a CRP of over 300 mg/L. There was no evidence of infection and his MRI was repeated which did not show any abnormal high signal on this occasion. His steroids were again increased. He was recommenced on MMF, which then had to be stopped owing to increased frequency of chest infections. He was noted to be Cushingoid as a result of prolonged steroid therapy. In May 2010 he was commenced on plasma exchange which, after seven exchanges, successfully treated ongoing symptoms of leg pain attributed to spinal vasculitis and brought his CRP to below 3 mg/L. Plasma exchange is being continued at present due to continued pANCA positivity.