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Sensory,psychological, and metabolic dysfunction in HIV-associated peripheral neuropathy: A cross-sectional deep profiling study
Authors:Tudor J.C. Phillips  Matthew Brown  Juan D. Ramirez  James Perkins  Yohannes W. Woldeamanuel  Amanda C. de C. Williams  Christine Orengo  David L.H. Bennett  Istvan Bodi  Sarah Cox  Christoph Maier  Elena K. Krumova  Andrew S.C. Rice
Affiliation:1. Pain Research Group, Department of Surgery and Cancer, Faculty of Medicine, Imperial College London, Chelsea and Westminster Hospital Campus, London, UK;2. Nuffield Department of Clinical Neurosciences, Oxford University, UK;3. Department of Bioinformatics, University College London, UK;4. Department of Neurology, Addis Ababa University School of Medicine, Addis Ababa, Ethiopia;5. Research Department of Clinical, Educational, and Health Psychology, University College London, UK;6. Department of Neuropathology, Kings College London, UK;g Pain Medicine, Chelsea and Westminster Hospital NHS Foundation Trust, London, UK;h Department of Pain Management, BG University Hospital, Bochum, Germany;i Department of Neurology, BG University Hospital, Bochum, Germany
Abstract:HIV-associated sensory neuropathy (HIV-SN) is a frequent complication of HIV infection and a major source of morbidity. A cross-sectional deep profiling study examining HIV-SN was conducted in people living with HIV in a high resource setting using a battery of measures which included the following: parameters of pain and sensory symptoms (7 day pain diary, Neuropathic Pain Symptom Inventory [NPSI] and Brief Pain Inventory [BPI]), sensory innervation (structured neurological examination, quantitative sensory testing [QST] and intraepidermal nerve fibre density [IENFD]), psychological state (Pain Anxiety Symptoms Scale-20 [PASS-20], Depression Anxiety and Positive Outlook Scale [DAPOS], and Pain Catastrophizing Scale [PCS], insomnia (Insomnia Severity Index [ISI]), and quality of life (Short Form (36) Health Survey [SF-36]). The diagnostic utility of the Brief Peripheral Neuropathy Screen (BPNS), Utah Early Neuropathy Scale (UENS), and Toronto Clinical Scoring System (TCSS) were evaluated. Thirty-six healthy volunteers and 66 HIV infected participants were recruited. A novel triumvirate case definition for HIV-SN was used that required 2 out of 3 of the following: 2 or more abnormal QST findings, reduced IENFD, and signs of a peripheral neuropathy on a structured neurological examination. Of those with HIV, 42% fulfilled the case definition for HIV-SN (n = 28), of whom 75% (n = 21) reported pain. The most frequent QST abnormalities in HIV-SN were loss of function in mechanical and vibration detection. Structured clinical examination was superior to QST or IENFD in HIV-SN diagnosis. HIV-SN participants had higher plasma triglyceride, concentrations depression, anxiety and catastrophizing scores, and prevalence of insomnia than HIV participants without HIV-SN.
Keywords:Anxiety   Catastrophizing   Depression   Diagnosis   HIV-SN   IENFD   Pain   Phenotyping   QST   Quality of life   Triglycerides
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