Your search keyword '"Peripheral Neuropathy"' showing total 796 results

1. Elevated Biomarkers of Inflammation and Vascular Dysfunction Are Associated with Distal Sensory Polyneuropathy in People with HIV

Author

Andalibi, Mohammadsobhan Sheikh, Andalibi, Mohammadsobhan Sheikh, Fields, Jerel Adam, Iudicello, Jennifer E, Diaz, Monica M, Tang, Bin, Letendre, Scott L, Ellis, Ronald J, Andalibi, Mohammadsobhan Sheikh, Andalibi, Mohammadsobhan Sheikh, Fields, Jerel Adam, Iudicello, Jennifer E, Diaz, Monica M, Tang, Bin, Letendre, Scott L, and Ellis, Ronald J

Abstract

Distal sensory polyneuropathy (DSP) is a disabling, chronic condition in people with HIV (PWH), even those with viral suppression of antiretroviral therapy (ART), and with a wide range of complications, such as reduced quality of life. Previous studies demonstrated that DSP is associated with inflammatory cytokines in PWH. Adhesion molecules, essential for normal vascular function, are perturbed in HIV and other conditions linked to DSP, but the link between adhesion molecules and DSP in PWH is unknown. This study aimed to determine whether DSP signs and symptoms were associated with a panel of plasma biomarkers of inflammation (d-dimer, sTNFRII, MCP-1, IL-6, IL-8, IP-10, sCD14) and vascular I integrity (ICAM-1, VCAM-1, uPAR, MMP-2, VEGF, uPAR, TIMP-1, TIMP-2) and differed between PWH and people without HIV (PWoH). A cross-sectional study was conducted among 143 participants (69 PWH and 74 PWoH) assessed by studies at the UC San Diego HIV Neurobehavioral Research Program. DSP signs and symptoms were clinically assessed for all participants. DSP was defined as two or more DSP signs: bilateral symmetrically reduced distal vibration, sharp sensation, and ankle reflexes. Participant-reported symptoms were neuropathic pain, paresthesias, and loss of sensation. Factor analyses reduced the dimensionality of the 15 biomarkers among all participants, yielding six factors. Logistic regression was used to assess the associations between biomarkers and DSP signs and symptoms, controlling for relevant demographic and clinical covariates. The 143 participants were 48.3% PWH, 47 (32.9%) women, and 47 (33.6%) Hispanics, with a mean age of 44.3 ± 12.9 years. Among PWH, the median (IQR) nadir and current CD4+ T-cells were 300 (178-448) and 643 (502-839), respectively. Participants with DSP were older but had similar distributions of gender and ethnicity to those without DSP. Multiple logistic regression showed that Factor 2 (sTNFRII and VCAM-1) and Factor 4 (MMP-2) were independently

Published

2024

2. Use of corticosteroids for adult chronic pain interventions: sympathetic and peripheral nerve blocks, trigger point injections - guidelines from the American Society of Regional Anesthesia and Pain Medicine, the American Academy of Pain Medicine, the American Society of Interventional Pain Physicians, the International Pain and Spine Intervention Society, and the North American Spine Society

Author

Benzon, Honorio T, Benzon, Honorio T, Elmofty, Dalia, Shankar, Hariharan, Rana, Maunak, Chadwick, Andrea L, Shah, Shalini, Souza, Dmitri, Nagpal, Ameet S, Abdi, Salahadin, Rafla, Christian, Abd-Elsayed, Alaa, Doshi, Tina L, Eckmann, Maxim S, Hoang, Thanh D, Hunt, Christine, Pino, Carlos A, Rivera, Jessica, Schneider, Byron J, Stout, Alison, Stengel, Angela, Mina, Maged, FitzGerald, John D, Hirsch, Joshua A, Wasan, Ajay D, Manchikanti, Laxmaiah, Provenzano, David Anthony, Narouze, Samer, Cohen, Steven P, Maus, Timothy P, Nelson, Ariana M, Shanthanna, Harsha, Benzon, Honorio T, Benzon, Honorio T, Elmofty, Dalia, Shankar, Hariharan, Rana, Maunak, Chadwick, Andrea L, Shah, Shalini, Souza, Dmitri, Nagpal, Ameet S, Abdi, Salahadin, Rafla, Christian, Abd-Elsayed, Alaa, Doshi, Tina L, Eckmann, Maxim S, Hoang, Thanh D, Hunt, Christine, Pino, Carlos A, Rivera, Jessica, Schneider, Byron J, Stout, Alison, Stengel, Angela, Mina, Maged, FitzGerald, John D, Hirsch, Joshua A, Wasan, Ajay D, Manchikanti, Laxmaiah, Provenzano, David Anthony, Narouze, Samer, Cohen, Steven P, Maus, Timothy P, Nelson, Ariana M, and Shanthanna, Harsha

Abstract

BackgroundThere is potential for adverse events from corticosteroid injections, including increase in blood glucose, decrease in bone mineral density and suppression of the hypothalamic-pituitary axis. Published studies note that doses lower than those commonly injected provide similar benefit.MethodsDevelopment of the practice guideline was approved by the Board of Directors of American Society of Regional Anesthesia and Pain Medicine with several other societies agreeing to participate. The scope of guidelines was agreed on to include safety of the injection technique (landmark-guided, ultrasound or radiology-aided injections); effect of the addition of the corticosteroid on the efficacy of the injectate (local anesthetic or saline); and adverse events related to the injection. Based on preliminary discussions, it was decided to structure the topics into three separate guidelines as follows: (1) sympathetic, peripheral nerve blocks and trigger point injections; (2) joints; and (3) neuraxial, facet, sacroiliac joints and related topics (vaccine and anticoagulants). Experts were assigned topics to perform a comprehensive review of the literature and to draft statements and recommendations, which were refined and voted for consensus (≥75% agreement) using a modified Delphi process. The United States Preventive Services Task Force grading of evidence and strength of recommendation was followed.ResultsThis guideline deals with the use and safety of corticosteroid injections for sympathetic, peripheral nerve blocks and trigger point injections for adult chronic pain conditions. All the statements and recommendations were approved by all participants after four rounds of discussion. The Practice Guidelines Committees and Board of Directors of the participating societies also approved all the statements and recommendations. The safety of some procedures, including stellate blocks, lower extremity peripheral nerve blocks and some sites of trigger point injections, is impro

Published

2024

3. Actividad Electrodérmica como Indicador Preventivo de Complicaciones por Neuropatía Periférica

Author

Universidad de Alicante. Departamento de Ingeniería Civil, Romero-Ante, Juan David, Vicente-Samper, Jose Maria, Manrique-Córdoba, Juliana, Esteve-Sala, Vicente, Casa Lillo, Miguel Ángel de la, Sabater Navarro, José María, Universidad de Alicante. Departamento de Ingeniería Civil, Romero-Ante, Juan David, Vicente-Samper, Jose Maria, Manrique-Córdoba, Juliana, Esteve-Sala, Vicente, Casa Lillo, Miguel Ángel de la, and Sabater Navarro, José María

Abstract

La neuropatía periférica (NP) es una afección causada por el daño a los nervios periféricos, responsables del movimiento de los brazos y piernas. La NP puede afectar los nervios autónomos, alterando la función sudomotora y generando piel seca y agrietada. Este artículo explora el uso de las propiedades eléctricas de la piel para medir la actividad electrodérmica (EDA) y su utilidad en la evaluación del grado de afectación de la NP. Se ofrece una visión general de la NP y las características de la señal de EDA, así como algunos modelos eléctricos utilizados para su medición. Además, se revisan estudios que relacionan la EDA con el nivel de afectación del paciente. Finalmente, se presenta el diseño de un circuito electrónico para medir la EDA, con el objetivo de desarrollar un sistema portátil capaz de monitorizar en tiempo real la conductancia eléctrica de la piel en la planta del pie, facilitando el seguimiento a nivel ambulatorio de los pacientes., Peripheral neuropathy (PN) is a condition caused by damage to the peripheral nerves responsible for arm and leg movement. PN can affect autonomic nerves, impair sudomotor function, and cause dryness and cracking of the skin. This article explores the use of the electrical properties of the skin to measure electrodermal activity (EDA) and its usefulness in assessing the degree of PN involvement. An overview of PN and the characteristics of the EDA signal are provided, as well as some electrical models used for its measurement. In addition, studies relating EDA to the patient’s level of impairment are reviewed. Finally, the design of an electronic circuit for measuring EDA is presented, with the aim of developing a portable system capable of monitoring in real time the electrical conductance of the skin on the sole of the foot, facilitating the outpatient follow-up of patients.

Published

2024

4. Análisis de presión plantar para el diseño de plantillas personalizadas

Author

Universidad de Alicante. Departamento de Ingeniería Civil, Romero-Ante, Juan David, Montenegro-Bravo, Juan Sebastián, Rodriguez-Lopez, Daniel Alejandro, Vicente-Samper, Jose Maria, Rodríguez-Martínez, A., Sabater Navarro, José María, Universidad de Alicante. Departamento de Ingeniería Civil, Romero-Ante, Juan David, Montenegro-Bravo, Juan Sebastián, Rodriguez-Lopez, Daniel Alejandro, Vicente-Samper, Jose Maria, Rodríguez-Martínez, A., and Sabater Navarro, José María

Abstract

La enfermedad arterial periférica (EAP) se caracteriza por la obstrucción de las arterias de las piernas y los pies debido a la acumulación de grasa. La neuropatía periférica (NP) afecta a la función de los nervios, incluidos los responsables de regular la sudoración y la humedad de los pies. Estos problemas aumentan significativamente el riesgo de úlceras y heridas en las extremidades. Este artículo presenta una metodología de análisis de la presión plantar con el equipo F-Scan64 para identificar puntos críticos durante las actividades diarias. El objetivo es diseñar plantillas personalizadas que monitoricen estos puntos y reduzcan el riesgo de lesiones en pacientes con estas afecciones. Los resultados se discuten en relación con estudios previos sobre los umbrales de riesgo que deben evitarse en estos casos. Además, se ofrece una perspectiva sobre la distribución sensorial de las plantillas personalizadas., Peripheral arterial disease (PAD) is characterized by blockage of the arteries in the legs and feet due to fatty deposits. Peripheral neuropathy (PN) affects the function of nerves, including those responsible for regulating sweat and moisture in the feet. These problems significantly increase the risk of ulcers and wounds in the extremities. This article presents a methodology for plantar pressure analysis using the F-Scan64 device to identify critical points during daily activities. The goal is to design customized insoles that monitor these points and reduce the risk of injury in patients with these conditions. The results are discussed in relation to previous studies on risk thresholds to avoid in these cases. In addition, a perspective on the sensory distribution of customized insoles is provided.

Published

2024

5. In vitro neurotoxicity testing: lessons from chemotherapy-induced peripheral neurotoxicity

Author

Tarasiuk, O, Invernizzi, C, Alberti, P, Tarasiuk, Olga, Invernizzi, Chiara, Alberti, Paola, Tarasiuk, O, Invernizzi, C, Alberti, P, Tarasiuk, Olga, Invernizzi, Chiara, and Alberti, Paola

Abstract

Introduction: Chemotherapy induced peripheral neurotoxicity (CIPN) is a long-lasting, or even permanent, late toxicity caused by largely used anticancer drugs. CIPN affects a growing population of cancer survivors and diminishes their quality of life since there is no curative/preventive treatment. Among several reasons for this unmet clinical need, there is an incomplete knowledge on mechanisms leading to CIPN. Therefore, bench side research is still greatly needed: in vitro studies are pivotal to both evaluate neurotoxicity mechanisms and potential neuroprotection strategies. Areas covered: Advantages and disadvantages of in vitro approaches are addressed with respect to their applicability to the CIPN field. Different cell cultures and techniques to assess neurotoxicity/neuroprotection are described. PubMed search-string: (chemotherapy-induced) AND (((neuropathy) OR neurotoxicity) OR neuropathic pain) AND (in vitro) AND (((((model) OR SH-SY5Y) OR PC12) OR iPSC) OR DRG neurons); (chemotherapy-induced) AND (((neuropathy) OR neurotoxicity) OR neuropathic pain) AND (model) AND (((neurite elongation) OR cell viability) OR morphology). No articles published before 1990 were selected. Expert opinion: CIPN is an ideal experimental setting to test axonal damage and, in general, peripheral nervous system mechanisms of disease and neuroprotection. Therefore, starting from robust preclinical data in this field, potentially, relevant biological rationale can be transferred to other human spontaneous diseases of the peripheral nervous system.

Published

2024

6. A muscarinic receptor antagonist reverses multiple indices of diabetic peripheral neuropathy: preclinical and clinical studies using oxybutynin

Author

Casselini, Carolina M, Casselini, Carolina M, Parson, Henri K, Frizzi, Katie E, Marquez, Alex, Smith, Darrell R, Guernsey, Lucie, Nemmani, Rakesh, Tayarani, Alireza, Jolivalt, Corinne G, Weaver, Jessica, Fernyhough, Paul, Vinik, Aaron I, Calcutt, Nigel A, Casselini, Carolina M, Casselini, Carolina M, Parson, Henri K, Frizzi, Katie E, Marquez, Alex, Smith, Darrell R, Guernsey, Lucie, Nemmani, Rakesh, Tayarani, Alireza, Jolivalt, Corinne G, Weaver, Jessica, Fernyhough, Paul, Vinik, Aaron I, and Calcutt, Nigel A

Abstract

Preclinical studies indicate that diverse muscarinic receptor antagonists, acting via the M1 sub-type, promote neuritogenesis from sensory neurons in vitro and prevent and/or reverse both structural and functional indices of neuropathy in rodent models of diabetes. We sought to translate this as a potential therapeutic approach against structural and functional indices of diabetic neuropathy using oxybutynin, a muscarinic antagonist approved for clinical use against overactive bladder. Studies were performed using sensory neurons maintained in vitro, rodent models of type 1 or type 2 diabetes and human subjects with type 2 diabetes and confirmed neuropathy. Oxybutynin promoted significant neurite outgrowth in sensory neuron cultures derived from adult normal rats and STZ-diabetic mice, with maximal efficacy in the 1-100 nmol/l range. This was accompanied by a significantly enhanced mitochondrial energetic profile as reflected by increased basal and maximal respiration and spare respiratory capacity. Systemic (3-10 mg/kg/day s.c.) and topical (3% gel daily) oxybutynin reversed paw heat hypoalgesia in the STZ and db/db mouse models of diabetes and reversed paw tactile allodynia in STZ-diabetic rats. Loss of nerve profiles in the skin and cornea of db/db mice was also prevented by daily topical delivery of 3% oxybutynin for 8 weeks. A randomized, double-blind, placebo-controlled interventional trial was performed in subjects with type 2 diabetes and established peripheral neuropathy. Subjects received daily topical treatment with 3% oxybutynin gel or placebo for 6 months. The a priori designated primary endpoint, significant change in intra-epidermal nerve fibre density (IENFD) in skin biopsies taken before and after 20 weeks of treatments, was met by oxybutynin but not placebo. Secondary endpoints showing significant improvement with oxybutynin treatment included scores on clinical neuropathy, pain and quality of life scales. This proof-o

Published

2024

7. Post-surgical inflammatory neuropathy after anterior cruciate ligament repair: a case report.

Author

Sun, Lisa, Sun, Lisa, Gray, Andrew, Braehler, Matthias, Sun, Lisa, Sun, Lisa, Gray, Andrew, and Braehler, Matthias

Abstract

BACKGROUND: Unanticipated symptoms of peripheral nerve damage following surgery are distressing to both the patient and their clinical team, including surgeons, anesthesiologists, and neurologists. The causes that are commonly considered for perioperative neuropathy can include surgical trauma, positioning-related injury, or injury related to a regional anesthetic technique. However, these cases often do not have a clear etiology and can occur without any apparent periprocedural anomalies. Postoperative inflammatory neuropathy is a more recently described, and potentially underrecognized cause of perioperative neuropathy which may improve with corticosteroid therapy. Therefore, it is an important etiology to consider early in the evaluation of perioperative neuropathy. CASE PRESENTATION: An otherwise healthy patient presented for left anterior cruciate ligament reconstruction. He underwent femoral and sciatic ultrasound-guided single-injection peripheral nerve blocks preoperatively, followed by a general anesthetic for the surgical procedure. He developed postoperative neuropathy in the sciatic distribution with both sensory and motor deficits. The patient received multi-disciplinary consultations, including neurology and pain management, and a broad differential diagnosis was considered. Based on neurological evaluation and imaging studies, a final diagnosis of post-surgical inflammatory neuropathy was made. The patients course improved with conservative management, but immunosuppressive treatment may have been considered for a more severe or worsening clinical course. CONCLUSIONS: There are limited publications describing postoperative inflammatory neuropathy, and this case serves to illustrate a potentially under-recognized and multifactorial cause of postoperative neuropathy. Perioperative neuropathies are a complication that surgeons and anesthesiologists strive to avoid; however, prevention and treatment of this condition have been elusive. Increased reporting

Published

2024

8. HbA1c and the risk of developing peripheral neuropathy in childhood-onset type 1 diabetes : A follow-up study over 3 decades

Author

Baldimtsi, Evangelia, Amezcua, Salvador, Ulander, Martin, Hyllienmark, Lars, Olausson, Håkan, Ludvigsson, Johnny, Wahlberg, Jeanette, Baldimtsi, Evangelia, Amezcua, Salvador, Ulander, Martin, Hyllienmark, Lars, Olausson, Håkan, Ludvigsson, Johnny, and Wahlberg, Jeanette

Abstract

AIMS: We have evaluated long-term weighted mean HbA1c (wHbA1c), HbA1c variability, diabetes duration, and lipid profiles in relation to the development of diabetic peripheral neuropathy (DPN), nephropathy, and retinopathy in childhood-onset type 1 diabetes. MATERIALS AND METHODS: In a longitudinal cohort study, 49 patients (21 women) with childhood-onset type 1 diabetes were investigated with neurophysiological measurements, blood tests, and clinical examinations after a diabetes duration of 7.7 (±3.3) years (baseline) and followed with repeated examinations for 30.6 (±5.2) years. We calculated wHbA1c by integrating the area under all HbA1c values since the diabetes diagnosis. Lipid profiles were analysed in relation to the presence of DPN. Long-term fluctuations of HbA1c variability were computed as the standard deviation of all HbA1c measurements. Data regarding the presence of other diabetes complications were retrieved from medical records. RESULTS: In this follow-up study, 51% (25/49) of the patients fulfilled electrophysiological criteria for DPN. In nerve conduction studies, there was a deterioration in the amplitudes and conduction velocities for the median, peroneal, and sural nerves over time. Patients with DPN had a longer duration of diabetes, higher wHbA1c, and increased HbA1c variability. The lowest wHbA1c value associated with the development of DPN was 62 mmol/mol (7.8%). The presence of albuminuria and retinopathy was positively correlated with the presence of neuropathy. CONCLUSIONS: More than half of the patients had developed DPN after 30 years. None of the patients who developed DPN had a wHbA1c of less than 62 mmol/mol (7.8%)., Financial support was received from Linköping University, Sweden, ALF grants (Swedish governmental funding of clinical research), and the Medical Research Council of Southeast Sweden.

Published

2024

9. Effects of vincristine and monosodium glutamate on gastrointestinal motility and visceral sensitivity

Author

Fundación Mapfre, Ministerio de Ciencia e Innovación (España), Comunidad de Madrid, Ministerio de Ciencia, Innovación y Universidades (España), Grupo Español de Motilidad Digestiva, Asociación Española de Gastroenterología, Universidad Rey Juan Carlos, Lopez-Tofiño, Yolanda, de Sosa, F., Vera, Gema, López-Gómez, L., Herradón, Esperanza, López-Miranda, Visitación, Nurgali, K., Uranga, J. A., Abalo, Raquel, Fundación Mapfre, Ministerio de Ciencia e Innovación (España), Comunidad de Madrid, Ministerio de Ciencia, Innovación y Universidades (España), Grupo Español de Motilidad Digestiva, Asociación Española de Gastroenterología, Universidad Rey Juan Carlos, Lopez-Tofiño, Yolanda, de Sosa, F., Vera, Gema, López-Gómez, L., Herradón, Esperanza, López-Miranda, Visitación, Nurgali, K., Uranga, J. A., and Abalo, Raquel

Abstract

Background: Chemotherapy-induced adverse effects are an unresolved nightmare. In preclinical studies in rats, the food additive monosodium glutamate (MSG) improved some of the side effects caused by cisplatin, but its effects in other models of chemotherapy-treated animals are not well known. The aim of this study was to test if MSG may improve some of the adverse effects induced by vincristine in rats. Methods: Young male Wistar rats were exposed or not to MSG (4 g L) in drinking water from week 0 till 1 week after treatment (week 3). Rats received two cycles of five daily intraperitoneal (ip) injections (Monday to Friday, weeks 1 and 2) of either saline (2 mL kg) or vincristine (0.1 mg kg). Gastrointestinal motility was measured in vivo by radiological methods after the first and tenth ip administrations. On week 3, the threshold for mechanical somatic and colorectal sensitivity was recorded using Von Frey filaments applied to the paws and an intracolonic balloon, respectively. Finally, samples of the terminal ileum and distal colon were histologically evaluated in sections. Key Results: Vincristine reduced body weight gain, food intake, and upper gastrointestinal transit, caused somatic (but not visceral) hypersensitivity and increased the thickness of the submucosal and muscle layers of the small intestine. In vincristine-treated animals, MSG partially prevented gastrointestinal dysmotility and reduced visceral sensitivity but did not improve structural alterations of the small intestine. Conclusions & Inferences: MSG could be used as an adjuvant to conventional treatments to improve some gastrointestinal dysfunctions caused by chemotherapy.

Published

2024

10. Association Between First-time Neurologic Events and Metronidazole Treatment:A Case-time Control Study

Author

Andersen, Michael Asger, Gregersen, Rasmus, Petersen, Tonny Studsgaard, Wang, Joanna Nan, Petersen, Janne, Jimenez-Solem, Espen, Andersen, Michael Asger, Gregersen, Rasmus, Petersen, Tonny Studsgaard, Wang, Joanna Nan, Petersen, Janne, and Jimenez-Solem, Espen

Abstract

Purpose: Metronidazole, a widely used antimicrobial medication, has been linked to neurologic adverse drug reactions. This study investigates the association between metronidazole use and first-time neurologic events. Methods: We conducted a case-time-control study using data from the Danish National Patient Register and the National Prescription Register in years 2013 to 2021. Patients with a first-time diagnosis of encephalopathy, cerebellar dysfunction, or peripheral neuropathy were included. Conditional logistic regression analyses were performed to estimate the risk of neurologic events associated with metronidazole use. Findings: Out of 476,066 first-time metronidazole prescriptions, the 100-day cumulative incidence of peripheral neuropathy was 0.016%, and 0.002% for cerebellar dysfunction or encephalopathy. In the case-time control study, we identified 17,667 persons with a first-time neurologic event and were included for the analysis. The estimated odds ratio for the combined neurologic events was 0.98 (95% CI, 0.59–1.64, P = 0.95) with no statistically significant association across different subgroups and time windows. Implications: Our findings suggest that metronidazole-induced neurologic events may be rarer than previously described, and we did not find any consistent or statistically significant association between metronidazole exposure. Nonetheless, clinicians should remain vigilant to potential neurologic risks in patients receiving metronidazole, to ensure its safe and effective use.

Published

2024

11. Targeted Sequencing Reveals Low-Frequency Variants in EPHA Genes as Markers of Paclitaxel-Induced Peripheral Neuropathy

Author

Apellániz Ruiz, María, Tejero Franco, Héctor, Inglada Pérez, Lucía Silvia, Sánchez Barroso, Lara, Gutiérrez Gutiérrez, Gerardo, Calvo, Isabel, Castelo, Beatriz, Redondo, Andrés, García Donás, Jesús, Romero Laorden, Nuria, Sereno, María, Merino, María, Currás Freixes, María, Montero Conde, Cristina, Mancikova, Veronika, Åvall Lundqvist, Elisabeth, Green, Henrik, Al-Shahrour, Fátima, Cascón, Alberto, Robledo, Mercedes, Rodríguez Antona, Cristina, Apellániz Ruiz, María, Tejero Franco, Héctor, Inglada Pérez, Lucía Silvia, Sánchez Barroso, Lara, Gutiérrez Gutiérrez, Gerardo, Calvo, Isabel, Castelo, Beatriz, Redondo, Andrés, García Donás, Jesús, Romero Laorden, Nuria, Sereno, María, Merino, María, Currás Freixes, María, Montero Conde, Cristina, Mancikova, Veronika, Åvall Lundqvist, Elisabeth, Green, Henrik, Al-Shahrour, Fátima, Cascón, Alberto, Robledo, Mercedes, and Rodríguez Antona, Cristina

Abstract

Purpose: Neuropathy is the dose-limiting toxicity of paclitaxel and a major cause for decreased quality of life. Genetic factors have been shown to contribute to paclitaxel neuropathy susceptibility; however, the major causes for interindividual differences remain unexplained. In this study, we identified genetic markers associated with paclitaxel-induced neuropathy through massive sequencing of candidate genes. Experimental Design: We sequenced the coding region of 4 EPHA genes, 5 genes involved in paclitaxel pharmacokinetics, and 30 Charcot–Marie–Tooth genes, in 228 cancer patients with no/low neuropathy or high-grade neuropathy during paclitaxel treatment. An independent validation series included 202 paclitaxel-treated patients. Variation-/gene-based analyses were used to compare variant frequencies among neuropathy groups, and Cox regression models were used to analyze neuropathy along treatment. Results: Gene-based analysis identified EPHA6 as the gene most significantly associated with paclitaxel-induced neuropathy. Low-frequency nonsynonymous variants in EPHA6 were present exclusively in patients with high neuropathy, and all affected the ligand-binding domain of the protein. Accumulated dose analysis in the discovery series showed a significantly higher neuropathy risk for EPHA5/6/8 low-frequency nonsynonymous variant carriers [HR, 14.60; 95% confidence interval (CI), 2.33–91.62; P ¼ 0.0042], and an independent cohort confirmed an increased neuropathy risk (HR, 2.07; 95% CI, 1.14–3.77; P ¼ 0.017). Combining the series gave an estimated 2.5-fold higher risk of neuropathy (95% CI, 1.46–4.31; P ¼ 9.1 10 4). Conclusions: This first study sequencing EPHA genes revealed that low-frequency variants in EPHA6, EPHA5, and EPHA8 contribute to the susceptibility to paclitaxel-induced neuropathy. Furthermore, EPHA's neuronal injury repair function suggests that these genes might constitute important neuropathy markers for many neurotoxic drugs., Depto. de Enfermería, Fac. de Enfermería, Fisioterapia y Podología, TRUE, pub

Published

2024

12. Assessment of corneal pathology using corneal confocal microscopy in peripheral neuropathies

Author

Ferdousi, Maryam, Boulton, Andrew, and Tavakoli, Mitra

Subjects

617.7, Peripheral neuropathy, Corneal Confocal Microscopy

Abstract

The validity of corneal confocal microscopy (CCM) in assessing peripheral neuropathy has been studied extensively in several studies with a large cohort of subjects with diabetes and in a handful of studies with small sample sizes in subjects with other systemic conditions. The non-invasive nature of this technique as well as its high reproducibility, moderate to high sensitivity and specificity, and ease of use make it an ideal biomarker for diagnosing onset, severity and progression of peripheral neuropathy. This thesis aims to further investigate the potential of CCM by evaluating abnormalities in the corneal sub-basal nerve plexus, Langerhans Cells (LCs) and epithelial cells in neuropathy related to diabetes and cancer. This thesis has established that evaluating the sub-basal nerve plexus in the centre and at the inferior whorl increases the diagnostic performance of CCM. In addition to diagnosing clinical and subclinical neuropathy in children and adults with diabetes CCM can also identify sub-clinical nerve damage in patients with upper gastrointestinal cancer and assess the effects of chemotherapy. CCM also identifies differences in small fibre pathology between diabetic patients with and without painful neuropathy. Although there was an increased prevalence and severity of dry eye and LCs' density, this was not related to an abnormality of corneal nerves in diabetic patients with no or mild neuropathy. Epithelial cell morphology was not associated with corneal nerve damage and did not alter in patients with Type 1 diabetes. In conclusion, CCM has been shown to be an ideal marker for quantifying early small fibre pathology and assessing peripheral neuropathies.

Published

2017

13. Derivation and Clinical Utility of Safety Targets for Linezolid-Related Adverse Events in Drug-Resistant Tuberculosis Treatment

Author

Keutzer, Lina, Mockeliunas, Laurynas, Sturkenboom, Marieke G. G., Bolhuis, Mathieu S., Akkerman, Onno W., Simonsson, Ulrika S. H., Keutzer, Lina, Mockeliunas, Laurynas, Sturkenboom, Marieke G. G., Bolhuis, Mathieu S., Akkerman, Onno W., and Simonsson, Ulrika S. H.

Abstract

Long-term usage of linezolid can result in adverse events such as peripheral neuropathy, anemia and thrombocytopenia. Therapeutic drug monitoring data from 75 drug-resistant tuberculosis patients treated with linezolid were analyzed using a time-to-event (TTE) approach for peripheral neuropathy and anemia and indirect response modelling for thrombocytopenia. Different time-varying linezolid pharmacokinetic exposure indices (AUC0-24h,ss, Cav, Cmax and Cmin) and patient characteristics were investigated as risk factors. A treatment duration shorter than 3 months was considered dropout and was modelled using a TTE approach. An exposure-response relationship between linezolid Cmin and both peripheral neuropathy and anemia was found. The exposure index which best described the development of thrombocytopenia was AUC0-24h. The final TTE dropout model indicated an association between linezolid Cmin and dropout. New safety targets for each adverse event were proposed which can be used for individualized linezolid dosing. According to the model predictions at 6 months of treatment, a Cmin of 0.11 mg/L and 1.4 mg/L should not be exceeded to keep the cumulative probability to develop anemia and peripheral neuropathy below 20%. The AUC0-24h should be below 111 h center dot mg/L or 270 h center dot mg/L to prevent thrombocytopenia and severe thrombocytopenia, respectively. A clinical utility assessment showed that the currently recommended dose of 600 mg once daily is safer compared to a 300 mg BID dosing strategy considering all four safety endpoints.

Published

2023

14. ACVR1-activating mutation causes neuropathic pain and sensory neuron hyperexcitability in humans.

Author

Yu, Xiaobing, Yu, Xiaobing, Ton, Amy N, Niu, Zejun, Morales, Blanca M, Chen, Jiadong, Braz, Joao, Lai, Michael H, Barruet, Emilie, Liu, Hongju, Cheung, Kin, Ali, Syed, Chan, Tea, Bigay, Katherine, Ho, Jennifer, Nikolli, Ina, Hansberry, Steven, Wentworth, Kelly, Kriegstein, Arnold, Basbaum, Allan, Hsiao, Edward C, Yu, Xiaobing, Yu, Xiaobing, Ton, Amy N, Niu, Zejun, Morales, Blanca M, Chen, Jiadong, Braz, Joao, Lai, Michael H, Barruet, Emilie, Liu, Hongju, Cheung, Kin, Ali, Syed, Chan, Tea, Bigay, Katherine, Ho, Jennifer, Nikolli, Ina, Hansberry, Steven, Wentworth, Kelly, Kriegstein, Arnold, Basbaum, Allan, and Hsiao, Edward C

Abstract

Altered bone morphogenetic protein (BMP) signaling is associated with many musculoskeletal diseases. However, it remains unknown whether BMP dysfunction has direct contribution to debilitating pain reported in many of these disorders. Here, we identified a novel neuropathic pain phenotype in patients with fibrodysplasia ossificans progressiva (FOP), a rare autosomal-dominant musculoskeletal disorder characterized by progressive heterotopic ossification. Ninety-seven percent of these patients carry an R206H gain-of-function point mutation in the BMP type I receptor ACVR1 (ACVR1 R206H ), which causes neofunction to Activin A and constitutively activates signaling through phosphorylated SMAD1/5/8. Although patients with FOP can harbor pathological lesions in the peripheral and central nervous system, their etiology and clinical impact are unclear. Quantitative sensory testing of patients with FOP revealed significant heat and mechanical pain hypersensitivity. Although there was no major effect of ACVR1 R206H on differentiation and maturation of nociceptive sensory neurons (iSNs) derived from FOP induced pluripotent stem cells, both intracellular and extracellular electrophysiology analyses of the ACVR1 R206H iSNs displayed ACVR1-dependent hyperexcitability, a hallmark of neuropathic pain. Consistent with this phenotype, we recorded enhanced responses of ACVR1 R206H iSNs to TRPV1 and TRPA1 agonists. Thus, activated ACVR1 signaling can modulate pain processing in humans and may represent a potential target for pain management in FOP and related BMP pathway diseases.

Published

2023

15. Initial observations on sexual dysfunction as a symptom of chemotherapy-induced peripheral neuropathy

Author

Reimer, N, Brodesser, D, Ratiu, D, Zubac, D, Lehmann, HC, Baumann, FT, Reimer, N, Brodesser, D, Ratiu, D, Zubac, D, Lehmann, HC, and Baumann, FT

Abstract

Introduction: Peripheral neuropathy (PNP) in feet and/or hands and sexual dysfunction are common side effects of cancer therapies. In patients with other diseases, there is evidence of an association between peripheral nervous system disorders and sexual dysfunction due to the impact of impaired neuronal control on genital organ sensitivity. In cancer patient interviews, it has now been observed that PNP and sexual dysfunction may be related. The aim of the study was to investigate the potential association between PNP, sexual dysfunction, and physical activity behavior.Methods: Ninety-three patients with PNP of the feet and/or hands were interviewed in August/September 2020 in a cross-sectional study regarding medical history, sexual dysfunction and functionality of the genital organs.Results: Thirty-one persons who participated in the survey provided seventeen evaluable questionnaires (four men, thirteen women). Nine women (69%) and three men (75%) reported sensory disorders of the genital organs. Three men (75%) had erectile dysfunction. All men who had sensory symptoms of the genital organs received chemotherapy, and one man also received immunotherapy. Eight women were sexually active. Five (63%) of them reported genital organ symptoms and mainly lubrication disorders. Four (80%) of the five sexually inactive women reported genital organ symptoms. Eight of the nine women with sensory symptoms of the genital organs received chemotherapy, and one woman received immunotherapy. Discussion: Our limited data suggest genital organ sensory symptoms in chemotherapy and immunotherapy patients. Genital organ symptoms do not appear to be directly related to sexual dysfunction, and the association between PNP and genital organ symptoms appears to be more pronounced in sexually inactive women. Chemotherapy could cause sensory symptoms of the genital organs and sexual dysfunction by damaging genital organ nerve fibers. Chemotherapy and anti-hormone therapy (AHT) could trigger, Einleitung: Polyneuropathie (PNP) in Füßen und/oder Händen und sexuelle Dysfunktion sind häufige Nebenwirkungen von Krebstherapien. Bei Patient*innen mit anderen Erkrankungen gibt es Hinweise auf einen Zusammenhang zwischen Erkrankungen des peripheren Nervensystems und der sexuellen Dysfunktion aufgrund des Einflusses der gestörten neuronalen Kontrolle auf die Sensibilität der Genitalorgane. In Gesprächen mit Krebspatient*innen wurde nun beobachtet, dass die PNP und die sexuelle Dysfunktion möglicherweise zusammenhängen. Ziel der Studie war, den potentiellen Zusammenhang zwischen PNP, sexueller Dysfunktion und körperlichem Aktivitätsverhalten zu untersuchen.Methoden: Dreiundneunzig Patient*innen mit PNP der Füße und/oder Hände wurden im August/September 2020 in einer Querschnittuntersuchung bezüglich Krankengeschichte, sexueller Dysfunktion und Funktionalität der Genitalorgane befragt.Ergebnisse: Einunddreißig Personen, die an der Umfrage teilnahmen, lieferten siebzehn auswertbare Fragebögen (vier Männer, dreizehn Frauen). Neun Frauen (69%) und drei Männer (75%) berichteten über Gefühlsstörungen an den Geschlechtsorganen. Drei Männer (75%) hatten eine erektile Dysfunktion. Alle Männer, die sensorische Beeinträchtigungen der Genitalorgane aufwiesen, erhielten Chemotherapie, und ein Mann zudem Immuntherapie. Acht Frauen waren sexuell aktiv. Fünf (63%) von ihnen berichteten von Symptomen der Genitalorgane und hauptsächlich Lubrikationsstörungen. Vier (80%) der fünf sexuell inaktiven Frauen berichteten von Symptomen der Genitalorgane. Acht der neun Frauen mit sensorischen Symptomen der Genitalorgane erhielten Chemotherapie und eine Frau erhielt Immuntherapie.Diskussion: Unsere begrenzten Daten deuten auf sensorische Symptome der Genitalorgane bei Chemotherapie- und Immuntherapie-Patient*innen hin. Symptome der Genitalorgane scheinen nicht direkt mit sexueller Dysfunktion zusammenzuhängen und der Zusammenhang zwischen PNP und Symptomen der Genitalorgane scheint bei sexue

Published

2023

16. Somatosensory Impairment and Chronic Pain Following Stroke: An Observational Study.

Author

Haslam, Brendon S, Haslam, Brendon S, Butler, David S, Kim, Anthony S, Carey, Leeanne M, Haslam, Brendon S, Haslam, Brendon S, Butler, David S, Kim, Anthony S, and Carey, Leeanne M

Abstract

BackgroundChronic pain and somatosensory impairment are common following a stroke. It is possible that an interaction exists between pain and somatosensory impairment and that a change in one may influence the other. We therefore investigated the presence of chronic pain and self-reported altered somatosensory ability in individuals with stroke, aiming to determine if chronic pain is more common in stroke survivors with somatosensory impairment than in those without.MethodsStroke survivors were invited to complete an online survey that included demographics, details of the stroke, presence of chronic pain, and any perceived changes in body sensations post-stroke.ResultsSurvivors of stroke (n = 489) completed the survey with 308 indicating that they experienced chronic pain and 368 reporting perceived changes in somatosensory function. Individuals with strokes who reported altered somatosensory ability were more likely to experience chronic pain than those who did not (OR = 1.697; 95% CI 1.585, 2.446). Further, this difference was observed for all categories of sensory function that were surveyed (detection of light touch, body position, discrimination of surfaces and temperature, and haptic object recognition).ConclusionsThe results point to a new characteristic of chronic pain in strokes, regardless of nature or region of the pain experienced, and raises the potential of somatosensory impairment being a rehabilitation target to improve pain-related outcomes for stroke survivors.

Published

2023

17. Insulin-regulated serine and lipid metabolism drive peripheral neuropathy.

Author

Handzlik, Michal K, Handzlik, Michal K, Gengatharan, Jivani M, Frizzi, Katie E, McGregor, Grace H, Martino, Cameron, Rahman, Gibraan, Gonzalez, Antonio, Moreno, Ana M, Green, Courtney R, Guernsey, Lucie S, Lin, Terry, Tseng, Patrick, Ideguchi, Yoichiro, Fallon, Regis J, Chaix, Amandine, Panda, Satchidananda, Mali, Prashant, Wallace, Martina, Knight, Rob, Gantner, Marin L, Calcutt, Nigel A, Metallo, Christian M, Handzlik, Michal K, Handzlik, Michal K, Gengatharan, Jivani M, Frizzi, Katie E, McGregor, Grace H, Martino, Cameron, Rahman, Gibraan, Gonzalez, Antonio, Moreno, Ana M, Green, Courtney R, Guernsey, Lucie S, Lin, Terry, Tseng, Patrick, Ideguchi, Yoichiro, Fallon, Regis J, Chaix, Amandine, Panda, Satchidananda, Mali, Prashant, Wallace, Martina, Knight, Rob, Gantner, Marin L, Calcutt, Nigel A, and Metallo, Christian M

Abstract

Diabetes represents a spectrum of disease in which metabolic dysfunction damages multiple organ systems including liver, kidneys and peripheral nerves1,2. Although the onset and progression of these co-morbidities are linked with insulin resistance, hyperglycaemia and dyslipidaemia3-7, aberrant non-essential amino acid (NEAA) metabolism also contributes to the pathogenesis of diabetes8-10. Serine and glycine are closely related NEAAs whose levels are consistently reduced in patients with metabolic syndrome10-14, but the mechanistic drivers and downstream consequences of this metabotype remain unclear. Low systemic serine and glycine are also emerging as a hallmark of macular and peripheral nerve disorders, correlating with impaired visual acuity and peripheral neuropathy15,16. Here we demonstrate that aberrant serine homeostasis drives serine and glycine deficiencies in diabetic mice, which can be diagnosed with a serine tolerance test that quantifies serine uptake and disposal. Mimicking these metabolic alterations in young mice by dietary serine or glycine restriction together with high fat intake markedly accelerates the onset of small fibre neuropathy while reducing adiposity. Normalization of serine by dietary supplementation and mitigation of dyslipidaemia with myriocin both alleviate neuropathy in diabetic mice, linking serine-associated peripheral neuropathy to sphingolipid metabolism. These findings identify systemic serine deficiency and dyslipidaemia as novel risk factors for peripheral neuropathy that may be exploited therapeutically.

Published

2023

18. Spinal disinhibition: evidence for a hyperpathia phenotype in painful diabetic neuropathy.

Author

Marshall, Anne, Marshall, Anne, Kalteniece, Alise, Ferdousi, Maryam, Azmi, Shazli, Jude, Edward B, Adamson, Clare, D'Onofrio, Luca, Dhage, Shaishav, Soran, Handrean, Campbell, Jackie, Lee-Kubli, Corinne A, Hamdy, Shaheen, Malik, Rayaz A, Calcutt, Nigel A, Marshall, Andrew G, Marshall, Anne, Marshall, Anne, Kalteniece, Alise, Ferdousi, Maryam, Azmi, Shazli, Jude, Edward B, Adamson, Clare, D'Onofrio, Luca, Dhage, Shaishav, Soran, Handrean, Campbell, Jackie, Lee-Kubli, Corinne A, Hamdy, Shaheen, Malik, Rayaz A, Calcutt, Nigel A, and Marshall, Andrew G

Abstract

The dominant sensory phenotype in patients with diabetic polyneuropathy and neuropathic pain is a loss of function. This raises questions as to which mechanisms underlie pain generation in the face of potentially reduced afferent input. One potential mechanism is spinal disinhibition, whereby a loss of spinal inhibition leads to increased ascending nociceptive drive due to amplification of, or a failure to suppress, incoming signals from the periphery. We aimed to explore whether a putative biomarker of spinal disinhibition, impaired rate-dependent depression of the Hoffmann reflex, is associated with a mechanistically appropriate and distinct pain phenotype in patients with painful diabetic neuropathy. In this cross-sectional study, 93 patients with diabetic neuropathy underwent testing of Hoffmann reflex rate-dependent depression and detailed clinical and sensory phenotyping, including quantitative sensory testing. Compared to neuropathic patients without pain, patients with painful diabetic neuropathy had impaired Hoffmann reflex rate-dependent depression at 1, 2 and 3 Hz (P ≤ 0.001). Patients with painful diabetic neuropathy exhibited an overall loss of function profile on quantitative sensory testing. However, within the painful diabetic neuropathy group, cluster analysis showed evidence of greater spinal disinhibition associated with greater mechanical pain sensitivity, relative heat hyperalgesia and higher ratings of spontaneous burning pain. These findings support spinal disinhibition as an important centrally mediated pain amplification mechanism in painful diabetic neuropathy. Furthermore, our analysis indicates an association between spinal disinhibition and a distinct phenotype, arguably akin to hyperpathia, with combined loss and relative gain of function leading to increasing nociceptive drive.

Published

2023

19. Continuous Ketamine Infusion as a Treatment for Refractory Facial Pain.

Author

Garcia, Roxana, Garcia, Roxana, Chen, QiLiang, Posadas, Edmund, Tran, Johnathan, Kwon, Albert, Qian, Xiang, Garcia, Roxana, Garcia, Roxana, Chen, QiLiang, Posadas, Edmund, Tran, Johnathan, Kwon, Albert, and Qian, Xiang

Abstract

Complex orofacial pain disorders, such as trigeminal neuralgia (TN) and atypical facial pain (AFP), can be excruciating and debilitating during attacks. Ketamine, an N-methyl-D-aspartate (NMDA) antagonist, is a powerful analgesic that has been used to treat various chronic pain conditions, but its role in treating complex facial pain has only been recently explored. In this retrospective case series, we reviewed the efficacy of continuous ketamine infusion for 12 patients with facial pain refractory to medical treatment. Patients who presented with a diagnosis of TN were more likely to have significant and sustained pain relief after receiving ketamine infusion. By contrast, those who did not respond to the treatment were more likely to have a diagnosis of AFP. The current report suggests a fundamental difference between these two facial pain disorders in their respective underlying pathophysiology and supports the use of continuous ketamine infusion for refractory TN, but not AFP.

Published

2023

20. Variant Sciatic Nerve Anatomy in Relation to the Piriformis Muscle on Magnetic Resonance Neurography: A Potential Etiology for Extraspinal Sciatica.

Author

Bharadwaj, Upasana Upadhyay, Bharadwaj, Upasana Upadhyay, Varenika, Vanja, Carson, William, Villanueva-Meyer, Javier, Ammanuel, Simon, Bucknor, Matthew, Robbins, Nathaniel M, Douglas, Vanja, Chin, Cynthia T, Bharadwaj, Upasana Upadhyay, Bharadwaj, Upasana Upadhyay, Varenika, Vanja, Carson, William, Villanueva-Meyer, Javier, Ammanuel, Simon, Bucknor, Matthew, Robbins, Nathaniel M, Douglas, Vanja, and Chin, Cynthia T

Abstract

ObjectiveTo assess the prevalence and clinical implications of variant sciatic nerve anatomy in relation to the piriformis muscle on magnetic resonance neurography (MRN), in patients with lumbosacral neuropathic symptoms.Materials and methodsIn this retrospective single-center study, 254 sciatic nerves, from 127 patients with clinical and imaging findings compatible with extra-spinal sciatica on MRN between 2003 and 2013, were evaluated for the presence and type of variant sciatic nerves, split sciatic nerve, abnormal T2-signal hyperintensity, asymmetric piriformis size and increased nerve caliber, and summarized using descriptive statistics. Two-tailed chi-square tests were performed to compare the anatomical variant type and clinical symptoms between imaging and clinical characteristics.ResultsSixty-four variant sciatic nerves were identified with an equal number of right and left variants. Bilateral variants were noted in 15 cases. Abnormal T2-signal hyperintensity was seen significantly more often in variant compared to conventional anatomy (40/64 vs. 82/190; p = 0.01). A sciatic nerve split was seen significantly more often in variant compared to conventional anatomy (56/64 vs. 20/190; p < 0.0001). Increased nerve caliber, abnormal T2-signal hyperintensity, and asymmetric piriformis size were significantly associated with the clinically symptomatic side compared to the asymptomatic side (98:2, 98:2, and 97:3, respectively; p < 0.0001 for all). Clinical symptoms were correlated with variant compared to conventional sciatic nerve anatomy (64% vs. 46%; p = 0.01).ConclusionVariant sciatic nerve anatomy, in relation to the piriformis muscle, is frequently identified with MRN and is more likely to be associated with nerve signal changes and symptomatology.

Published

2023

21. A multicentric study of the disease risks and first manifestations in Hereditary transthyretin amyloidosis (ATTRv) : insights for an earlier diagnosis

Author

Planté-Bordeneuve, Violaine, Gorram, Farida, Olsson, Malin, Anan, Intissar, Mazzeo, Anna, Gentile, Luca, Cisneros-Barroso, Eugenia, Gonzalez-Moreno, Juan, Losada, Ines, Waddington-Cruz, Marcia, Pinto, Luiz Felipe, Parman, Yeşim, Fanen, Pascale, Alarcon, Flora, Nuel, Gregory, Planté-Bordeneuve, Violaine, Gorram, Farida, Olsson, Malin, Anan, Intissar, Mazzeo, Anna, Gentile, Luca, Cisneros-Barroso, Eugenia, Gonzalez-Moreno, Juan, Losada, Ines, Waddington-Cruz, Marcia, Pinto, Luiz Felipe, Parman, Yeşim, Fanen, Pascale, Alarcon, Flora, and Nuel, Gregory

Abstract

Background: In hereditary transthyretin amyloidosis (ATTRv), early manifestation and age at onset (AO) may vary strikingly. We assessed the disease’risk (penetrance), AO and initial features in ATTRv families to gain insights on the early disease presentation. Methods: Genealogical information, AO and first disease manifestations were collected in ATTRv families, from Sweden, Italy (Sicily), Spain (Mallorca), France, Turkey, Brazil. Penetrance was computed using a non-parametric survival method. Results: We analysed 258 TTRV30M kindreds and 84 carrying six other variants (TTRT49A, F64L, S77Y, S77F, E89Q, I107V). In ATTRV30M families, the earliest disease risk was found at age 20 years in the Portuguese and Mallorcan families and at age 30-35 years, in the French and Swedish groups. The risks were higher in men and in carriers of maternal descent. In families carrying TTR-nonV30M variants, the earliest disease risk ranged from 30 y-o in TTRT49A to 55 y-o in TTRI107V families. Peripheral neuropathy symptoms were the most frequent initial manifestations. Among patients carrying TTRnonV30M variants, about 25% had an initial cardiac phenotype, one third a mixed phenotype. Conclusion: Our work provided solid data on the risks and early features of ATTRv in a spectrum of families to enhance an early diagnosis and treatment.

Published

2023

22. Collagen turnover is associated with cardiovascular autonomic and peripheral neuropathy in type 1 diabetes: novel pathophysiological mechanism?

Author

Hansen, Christian S., Rasmussen, Daniel G.K., Hansen, Tine W., Nielsen, Signe Holm, Theilade, Simone, Karsdal, Morten A., Genovese, Federica, Rossing, Peter, Hansen, Christian S., Rasmussen, Daniel G.K., Hansen, Tine W., Nielsen, Signe Holm, Theilade, Simone, Karsdal, Morten A., Genovese, Federica, and Rossing, Peter

Abstract

Background: Diabetic cardiovascular autonomic neuropathy (CAN) and distal symmetrical polyneuropathy (DSPN) are severe diabetic complications. Collagen type VI (COL6) and III (COL3) have been associated with nerve function. We investigated if markers of COL6 formation (PRO-C6) and COL3 degradation (C3M) were associated with neuropathy in people with type 1 diabetes (T1D). Methods: In a cross-sectional study including 300 people with T1D, serum and urine PRO-C6 and C3M were obtained. CAN was assessed by cardiovascular reflex tests: heart rate response to deep breathing (E/I ratio), to standing (30/15 ratio) and to the Valsalva maneuver (VM). Two or three pathological CARTs constituted CAN. DSPN was assessed by biothesiometry. Symmetrical vibration sensation threshold above 25 V constituted DSPN. Results: Participants were (mean (SD)) 55.7 (9.3) years, 51% were males, diabetes duration was 40.0 (8.9) years, HbA1c was 63 (11 mmol/mol, (median (IQR)) serum PRO-C6 was 7.8 (6.2;11.0) ng/ml and C3M 8.3 (7.1;10.0) ng/ml. CAN and DSPN were diagnosed in 34% and 43% of participants, respectively. In models adjusted for relevant confounders a doubling of serum PRO-C6, was significantly associated with odds ratio > 2 for CAN and > 1 for DSPN, respectively. Significance was retained after additional adjustments for eGFR only for CAN. Higher serum C3M was associated with presence of CAN, but not after adjustment for eGFR. C3M was not associated with DSPN. Urine PRO-C6 analyses indicated similar associations. Conclusions: Results show previously undescribed associations between markers of collagen turnover and risk of CAN and to a lesser degree DSPN in T1D.

Published

2023

23. Collagen turnover is associated with cardiovascular autonomic and peripheral neuropathy in type 1 diabetes:novel pathophysiological mechanism?

Author

Hansen, Christian S., Rasmussen, Daniel G.K., Hansen, Tine W., Nielsen, Signe Holm, Theilade, Simone, Karsdal, Morten A., Genovese, Federica, Rossing, Peter, Hansen, Christian S., Rasmussen, Daniel G.K., Hansen, Tine W., Nielsen, Signe Holm, Theilade, Simone, Karsdal, Morten A., Genovese, Federica, and Rossing, Peter

Abstract

Background: Diabetic cardiovascular autonomic neuropathy (CAN) and distal symmetrical polyneuropathy (DSPN) are severe diabetic complications. Collagen type VI (COL6) and III (COL3) have been associated with nerve function. We investigated if markers of COL6 formation (PRO-C6) and COL3 degradation (C3M) were associated with neuropathy in people with type 1 diabetes (T1D). Methods: In a cross-sectional study including 300 people with T1D, serum and urine PRO-C6 and C3M were obtained. CAN was assessed by cardiovascular reflex tests: heart rate response to deep breathing (E/I ratio), to standing (30/15 ratio) and to the Valsalva maneuver (VM). Two or three pathological CARTs constituted CAN. DSPN was assessed by biothesiometry. Symmetrical vibration sensation threshold above 25 V constituted DSPN. Results: Participants were (mean (SD)) 55.7 (9.3) years, 51% were males, diabetes duration was 40.0 (8.9) years, HbA1c was 63 (11 mmol/mol, (median (IQR)) serum PRO-C6 was 7.8 (6.2;11.0) ng/ml and C3M 8.3 (7.1;10.0) ng/ml. CAN and DSPN were diagnosed in 34% and 43% of participants, respectively. In models adjusted for relevant confounders a doubling of serum PRO-C6, was significantly associated with odds ratio > 2 for CAN and > 1 for DSPN, respectively. Significance was retained after additional adjustments for eGFR only for CAN. Higher serum C3M was associated with presence of CAN, but not after adjustment for eGFR. C3M was not associated with DSPN. Urine PRO-C6 analyses indicated similar associations. Conclusions: Results show previously undescribed associations between markers of collagen turnover and risk of CAN and to a lesser degree DSPN in T1D.

Published

2023

24. Toxic Medications in Charcot-Marie-Tooth Patients: A Systematic Review

Author

Cavaletti, G, Forsey, K, Alberti, P, Cavaletti, Guido, Forsey, Katherine, Alberti, Paola, Cavaletti, G, Forsey, K, Alberti, P, Cavaletti, Guido, Forsey, Katherine, and Alberti, Paola

Abstract

Background and Aims: Several widely used medications, with a relevant efficacy profile, are toxic to the peripheral nervous system and an even larger number of agents are suspected to be neurotoxic. There are concerns about the use of these drugs in patients with Charcot–Marie–Tooth disease (CMT), a hereditary motor and sensory neuropathy. This review provides evidence-based updated recommendations on this clinically relevant topic. Methods: A systematic review of the available studies/reports written in English was performed from July to September 2022 including in the search string all reported putative neurotoxic drugs. Results: The results of our systematic review provide evidence-based support for the statement that use of vincristine, and possibly paclitaxel, can occasionally induce an atypical, and more severe, course of drug-related peripheral neurotoxicity in CMT patients. It is therefore reasonable to recommend caution in the use of these compounds in CMT patients. However, no convincing evidence for a similar recommendation could be found for all other drugs. Interpretation: It is important that patients with CMT are not denied effective treatments that may prolong life expectancy for cancer or improve their health status if affected by non-oncological diseases. Accurate monitoring of peripheral nerve function in CMT patients treated with any neurotoxic agent remains mandatory to detect the earliest signs of neuropathy worsening and atypical clinical courses. Neurologists monitoring CMT patients as part of their normal care package or for natural history studies should keep detailed records of exposures to neurotoxic medications and support reporting of accelerated neuropathy progression if observed.

Published

2023

25. Paclitaxel, but Not Cisplatin, Affects Satellite Glial Cells in Dorsal Root Ganglia of Rats with Chemotherapy-Induced Peripheral Neurotoxicity

Author

Pozzi, E, Ballarini, E, Rodriguez Menendez, V, Canta, A, Chiorazzi, A, Monza, L, Bossi, M, Alberti, P, Malacrida, A, Meregalli, C, Scuteri, A, Cavaletti, G, Carozzi, V, Pozzi, E, Ballarini, E, Rodriguez Menendez, V, Canta, A, Chiorazzi, A, Monza, L, Bossi, M, Alberti, P, Malacrida, A, Meregalli, C, Scuteri, A, Cavaletti, G, and Carozzi, V

Abstract

Chemotherapy-induced peripheral neurotoxicity is one of the most common dose-limiting toxicities of several widely used anticancer drugs such as platinum derivatives (cisplatin) and taxanes (paclitaxel). Several molecular mechanisms related to the onset of neurotoxicity have already been proposed, most of them having the sensory neurons of the dorsal root ganglia (DRG) and the peripheral nerve fibers as principal targets. In this study we explore chemotherapy-induced peripheral neurotoxicity beyond the neuronocentric view, investigating the changes induced by paclitaxel (PTX) and cisplatin (CDDP) on satellite glial cells (SGC) in the DRG and their crosstalk. Rats were chronically treated with PTX (10 mg/Kg, 1qwx4) or CDDP (2 mg/Kg 2qwx4) or respective vehicles. Morpho-functional analyses were performed to verify the features of drug-induced peripheral neurotoxicity. Qualitative and quantitative immunohistochemistry, 3D immunofluorescence, immunoblotting, and transmission electron microscopy analyses were also performed to detect alterations in SGCs and their interconnections. We demonstrated that PTX, but not CDDP, produces a strong activation of SGCs in the DRG, by altering their interconnections and their physical contact with sensory neurons. SGCs may act as principal actors in PTX-induced peripheral neurotoxicity, paving the way for the identification of new druggable targets for the treatment and prevention of chemotherapy-induced peripheral neurotoxicity.

Published

2023

26. Multimodal Comparison of Diabetic Neuropathy in Aged Streptozotocin-Treated Sprague–Dawley and Zucker Diabetic Fatty Rats

Author

Canta, A, Carozzi, V, Chiorazzi, A, Meregalli, C, Oggioni, N, Rodriguez-Menendez, V, Sala, B, Melcangi, R, Giatti, S, Lombardi, R, Bianchi, R, Marmiroli, P, Cavaletti, G, Canta A., Carozzi V. A., Chiorazzi A., Meregalli C., Oggioni N., Rodriguez-Menendez V., Sala B., Melcangi R. C., Giatti S., Lombardi R., Bianchi R., Marmiroli P., Cavaletti G., Canta, A, Carozzi, V, Chiorazzi, A, Meregalli, C, Oggioni, N, Rodriguez-Menendez, V, Sala, B, Melcangi, R, Giatti, S, Lombardi, R, Bianchi, R, Marmiroli, P, Cavaletti, G, Canta A., Carozzi V. A., Chiorazzi A., Meregalli C., Oggioni N., Rodriguez-Menendez V., Sala B., Melcangi R. C., Giatti S., Lombardi R., Bianchi R., Marmiroli P., and Cavaletti G.

Abstract

The development and progression of diabetic polyneuropathy (DPN) are due to multiple mechanisms. The creation of reliable animal models of DPN has been challenging and this issue has not yet been solved. However, despite some recognized differences from humans, most of the current knowledge on the pathogenesis of DPN relies on results achieved using rodent animal models. The simplest experimental DPN model reproduces type 1 diabetes, induced by massive chemical destruction of pancreatic beta cells with streptozotocin (STZ). Spontaneous/transgenic models of diabetes are less frequently used, mostly because they are less predictable in clinical course, more expensive, and require a variable time to achieve homogeneous metabolic conditions. Among them, Zucker diabetic fatty (ZDF) rats represent a typical type 2 diabetes model. Both STZ-induced and ZDF rats have been extensively used, but only very few studies have compared the long-term similarities and differences existing between these two models. Moreover, inconsistencies have been reported regarding several aspects of short-term in vivo studies using these models. In this study, we compared the long-term course of DPN in STZ-treated Sprague–Dawley and ZDF rats with a multimodal set of readout measures.

Published

2023

27. Association between peripheral neuropathy and sleep quality among colorectal cancer patients from diagnosis until 2-year follow-up: Results from the PROFILES registry

Author

Bonhof, C., van de Poll-Franse, L.V., de Hingh, I.H.J.T., Nefs, G.M., Vreugdenhil, G., Mols, F., Bonhof, C., van de Poll-Franse, L.V., de Hingh, I.H.J.T., Nefs, G.M., Vreugdenhil, G., and Mols, F.

Abstract

Purpose Studies on the association between peripheral neuropathy (PN) and patient-reported outcomes have mostly overlooked sleep quality. Therefore, we aimed to assess the association between PN and sleep quality in a population-based sample of colorectal cancer (CRC) patients up two years after diagnosis. Methods All newly diagnosed CRC patients from four Dutch hospitals were eligible for participation. Patients (N=340) completed questionnaires about PN (EORTC QLQ-CIPN20) and sleep (PSQI) before initial treatment (baseline) and one and two years after diagnosis. Results Patients who developed sensory PN (n=76) or motor PN (n=79) after treatment more often reported poor sleeping scores (PSQI>5) compared with those who did not develop SPN or MPN at 1-year (SPN: 38% vs. 261%, MPN: 37% vs. 14%) and 2-year follow-up (SPN: 38 vs. 23%, MPN: 37% vs. 18%) (all p<0.05). Overall, results showed that among patients who did not develop SPN or MPN, sleep quality improved after baseline, while among patients with SPN or MPN, sleep quality did not improve at one and two years after diagnosis. Conclusions Both SPN and MPN were significantly associated with the course of sleep quality among CRC patients up to two years after diagnosis. Clinicians should be encouraged to discuss sleep quality with their patients who either report PN or are at risk of developing PN. Implications for survivors: Improving sleep quality among survivors with PN is important, either by reducing PN symptoms, or directly targeting sleep

Published

2023

28. The Spinal Cord in Diabetic Neuropathy

Author

Marshall, Andrew G, Marshall, Andrew G, Worthington, Anne, Jolivalt, Corinne G, Marshall, Andrew G, Marshall, Andrew G, Worthington, Anne, and Jolivalt, Corinne G

Published

2023

29. Effect of the Cannabinoid Agonist WIN 55,212-2 on Neuropathic and Visceral Pain Induced by a Non-Diarrheagenic Dose of the Antitumoral Drug 5-Fluorouracil in the Rat

Author

Ministerio de Ciencia, Innovación y Universidades (España), Vera, G., López-Gómez, L., Girón, R., Martín-Fontelles, M. I., Nurgali, K., Abalo, R., Uranga, J. A., Ministerio de Ciencia, Innovación y Universidades (España), Vera, G., López-Gómez, L., Girón, R., Martín-Fontelles, M. I., Nurgali, K., Abalo, R., and Uranga, J. A.

Abstract

5-fluorouracil (5-FU) is an antineoplastic drug used to treat colorectal cancer, but it causes, among other adverse effects, diarrhea and mucositis, as well as enteric neuropathy, as shown in experimental animals. It might also cause neuropathic pain and alterations in visceral sensitivity, but this has not been studied in either patients or experimental animals. Cannabinoids have antimotility and analgesic effects and may alleviate 5-FU-induced adverse effects. Our aim was to evaluate the effects of the cannabinoid agonist WIN 55,212-2 on neuropathic and visceral pain induced by a non-diarrheagenic dose of 5-FU. Male Wistar rats received a dose of 5-FU (150 mg/kg, ip) and gastrointestinal motility, colonic sensitivity, gut wall structure and tactile sensitivity were evaluated. WIN 55,212-2 (WIN) was administered to evaluate its effect on somatic (50–100 µg ipl; 1 mg/kg, ip) and visceral (1 mg/kg, ip) sensitivity. The cannabinoid tetrad was used to assess the central effects of WIN (1 mg/kg, ip). 5-FU decreased food intake and body weight gain, produced mucositis and thermal hyperalgesia, but these effects were reduced afterwards, and were not accompanied by diarrhea. Tactile mechanical allodynia was also evident and persisted for 15 days. Interestingly, it was alleviated by WIN. 5-FU tended to increase colonic sensitivity whereas WIN reduced the abdominal contractions induced by increasing intracolonic pressure in both control and 5-FU-treated animals. Importantly, the alleviating effects of WIN against those induced by 5-FU were not accompanied by any effect in the cannabinoid tetrad. The activation of the peripheral cannabinoid system may be useful to alleviate neuropathic and visceral pain associated with antitumoral treatment.

Published

2023

30. Peripheral and Cardiovascular Autonomic Neuropathy After Roux-en-Y Gastric Bypass Surgery:a Pilot Study

Author

Christensen, Marie Mathilde Bjerg, Hansen, Christian Stevns, Karlsson, Páll, Dirksen, Carsten, Christensen, Marie Mathilde Bjerg, Hansen, Christian Stevns, Karlsson, Páll, and Dirksen, Carsten

Abstract

Bariatric surgery (BS) effectively treats severe obesity and metabolic diseases [1], but carries a risk of impaired absorption of micronutrients (e.g., vitamins like D, B12, and thiamine, and trace elements like iron, zinc, copper, and calcium) [2] and increased postprandial glucose variability [3]. This is particularly true for BS procedures that involve intestinal bypass such as the widespread Roux-en-Y gastric bypass (RYGB) procedure. Therefore, patients with RYGB surgery are prone to complications such as iron deficiency anemia, insufficiency of vitamin D, B12 or thiamine, and post-bariatric hypoglycemia that often develop years after surgery [4, 5]. These deficiencies can cause a range of nerve dysfunctions [6,7,8], including peripheral neuropathy (PN) characterized by reduced sensation and pain in extremities [9], and autonomic neuropathy affecting the cardiovascular, gastrointestinal, urogenital, and sudomotor systems [10], but also nutrient deficiency specific conditions such as myelopathy (vitamin B12 and copper), Wernicke’s encephalopathy (thiamine), optic neuropathy, and spinocerebellar syndrome (vitamin E) [6]. Increased glycemic variability with hypoglycemic episodes may contribute to neuropathy development [11]. Thus, we hypothesize that BS patients, especially those with intestinal bypass that are prone to micronutrient malabsorption and with a history of longstanding nutritional deficiencies or hypoglycemic events, may be at increased risk of developing PN and autonomic neuropathy. Prior studies lack comprehensive and objective nerve function assessment, as well as long-term follow-up [7, 8, 12, 13]. In this cross-sectional pilot study, we assessed PN and cardiovascular autonomic neuropathy (CAN) in patients who had undergone RYGB more than 5 years ago and had suspected or confirmed nutritional and/or metabolic post-bariatric complications.

Published

2023

31. Nerve MR in the Differential Diagnosis of Neuropathies: A Case Series from a Single Center

Author

Giordano, Carolina, Sciarrone, Maria Ausilia, Vitali, Francesca, Romano, Angela, Guerri, Giulia, Perlangeli, Valentina, Gaudino, Simona, Luigetti, Marco, Gaudino, Simona (ORCID:0000-0003-1681-4343), Luigetti, Marco (ORCID:0000-0001-7539-505X), Giordano, Carolina, Sciarrone, Maria Ausilia, Vitali, Francesca, Romano, Angela, Guerri, Giulia, Perlangeli, Valentina, Gaudino, Simona, Luigetti, Marco, Gaudino, Simona (ORCID:0000-0003-1681-4343), and Luigetti, Marco (ORCID:0000-0001-7539-505X)

Abstract

In the present study, through a case series, we highlighted the role of magnetic resonance (MR) in the identification and diagnosis of peripheral neuropathies. MR neurography allows the evaluation of the course of nerves through 2D and 3D STIR sequences with an isotropic voxel, whereas the relationship between nerves, vessels, osteo-ligamentous and muscular structures can be appraised with T1 sequences. Currently, DTI and tractography are mainly used for experimental purposes. MR neurography can be useful in detecting subtle nerve alterations, even before the onset of symptoms. However, despite being sensitive, MR neurography is not specific in detecting nerve injury and requires careful interpretation. For this reason, MR information should always be supported by instrumental clinical tests.

Published

2023

32. Long-Term Health Effects of the 9/11 Disaster.

Author

Brackbill, Robert M., Graber, Judith M., and Robison, W. Allen

Subjects

9/11, 9/11 disaster, 9/11 impact, Asian Americans, Cox regression, FDNY, HQoL, PCL score, PTSD, PTSD cluster, PTSD symptom change, Scadding stage, Short Form-12 (SF-12), WTC, WTC attack, WTC responders, WTC survivors, WTC-related asthma, World Trade Center, World Trade Center (WTC), World Trade Center attack, World Trade Center disaster, World Trade Center exposure, aging, air pollution, airway hyperreactivity, airway physiology, allergen exposure, asthma, asthma control, asthma morbidity, asthma outcomes, asthma quality of life, biomarkers, cardiac sarcoidosis, chronic disease, chronic sinusitis, cleaning practices, cognitive decline, cognitive reserve, comorbid insomnia, counseling, depression, disaster, disaster epidemiology, disaster mental health, dust, environmental health, epidemiological studies, evidence-based treatment, extrathoracic sarcoidosis, fibrosis, fibrotic sarcoid, firefighters, forced oscillation, genetics, handgrip strength, hazard function, health insurance, health-related quality of life, immunoglobulin E, income loss, indoor allergens sensitization, inflammation, injury, irritant(s), latent class analysis, longitudinal analysis, lower Manhattan residents, lung function, lung injury, medical imaging, mental health, mental health conditions, mental health service use, mental health service utilization, mental health treatment, metabolic syndrome, mini asthma quality of life questionnaire, n/a, neuropathic symptoms, obstructive sleep apnea, occupational exposure, paresthesia, peripheral neuropathy, physical health, post-disaster, prevalence, psychotherapy, pulmonary fibrosis, pulmonary function tests, quality improvement, rescue/recovery workers, respiratory function, respiratory symptoms, retirement, sarcoidosis, screening, severe lung disease, sleep-related quality of life, sleepiness, small airway disease, social support, stressful life events, surveillance bias, thyroid cancer, treatment utilization, trigger(s), unmet mental health care needs

Abstract

Summary: The terrorist attacks on the World Trade Center towers on September 11, 2001, also referred as 9/11, was an iconic event in US history that altered the global and political response to terrorism. The attacks, which involved two planes hitting the twin towers in Lower Manhattan, New York City, resulted in the collapse of the buildings and over 2800 deaths of occupants of the buildings, fire, police and other responders and persons on the street in the vicinity of the collapsing buildings. The destroyed towers and the surrounding buildings have since been replaced but the health effects that resulted from the release of tons of dust, gases and debris as well as the life threat trauma are ongoing, and represent a major health burden among persons directly exposed. Hundreds of scientific publications have documented the physical and mental health effects attributed to the disaster. The current state-of-the-art in understanding the ongoing interactions of physical and mental health, especially PTSD, and the unique mechanisms by which pollutants from the building collapse, have resulted in long term pulmonary dysfunction, course of previously reported conditions, potential emerging conditions (e.g., heart disease and autoimmune diseases), as well as quality of life, functioning and unmet health care needs would be in the purview of this Special Issue on the 9/11 Disaster.

33. A human coronavirus OC43‐derived polypeptide causes neuropathic pain

Author

Shubayev, Veronica I, Shubayev, Veronica I, Dolkas, Jennifer, Catroli, Glaucilene Ferreira, Chernov, Andrei V, Shubayev, Veronica I, Shubayev, Veronica I, Dolkas, Jennifer, Catroli, Glaucilene Ferreira, and Chernov, Andrei V

Abstract

Human coronaviruses have been recently implicated in neurological sequelae by insufficiently understood mechanisms. We here identify an amino acid sequence within the HCoV-OC43 p65-like protein homologous to the evolutionarily conserved motif of myelin basic protein (MBP). Because MBP-derived peptide exposure in the sciatic nerve produces pronociceptive activity in female rodents, we examined whether a synthetic peptide derived from the homologous region of HCoV-OC43 (OC43p) acts by molecular mimicry to promote neuropathic pain. OC43p, but not scrambled peptides, induces mechanical hypersensitivity in rats following intrasciatic injections. Transcriptome analyses of the corresponding spinal cords reveal upregulation of genes and signaling pathways with known nociception-, immune-, and cellular energy-related activities. Affinity capture shows the association of OC43p with an Na+ /K+ -transporting ATPase, providing a potential direct target and mechanistic insight into virus-induced effects on energy homeostasis and the sensory neuraxis. We propose that HCoV-OC43 polypeptides released during infection dysregulate normal nervous system functions through molecular mimicry of MBP, leading to mechanical hypersensitivity. Our findings might provide a new paradigm for virus-induced neuropathic pain.

Published

2022

34. Chapter 13 Spinal GABA mechanism in neuropathic pain after spinal cord injury*

Author

Gwak, Young S, Gwak, Young S, Luo, Z David, Gwak, Young S, Gwak, Young S, and Luo, Z David

Published

2022

35. An ACVR1 activating mutation causes neuropathic pain and sensory neuron hyperexcitability in humans.

Author

Yu, Xiaobing, Yu, Xiaobing, Ton, Amy N, Niu, Zejun, Morales, Blanca M, Chen, Jiadong, Braz, Joao, Lai, Michael H, Barruet, Emilie, Liu, Hongju, Cheung, Kin, Ali, Syed, Chan, Tea, Bigay, Katherine, Ho, Jennifer, Nikolli, Ina, Hansberry, Steven, Wentworth, Kelly, Kriegstein, Arnold, Basbaum, Allan, Hsiao, Edward C, Yu, Xiaobing, Yu, Xiaobing, Ton, Amy N, Niu, Zejun, Morales, Blanca M, Chen, Jiadong, Braz, Joao, Lai, Michael H, Barruet, Emilie, Liu, Hongju, Cheung, Kin, Ali, Syed, Chan, Tea, Bigay, Katherine, Ho, Jennifer, Nikolli, Ina, Hansberry, Steven, Wentworth, Kelly, Kriegstein, Arnold, Basbaum, Allan, and Hsiao, Edward C

Abstract

Altered bone morphogenetic protein (BMP) signaling is associated with many musculoskeletal diseases. However, it remains unknown whether BMP dysfunction has direct contribution to debilitating pain reported in many of these disorders. Here we identified a novel neuropathic pain phenotype in patients with fibrodysplasia ossificans progressiva (FOP), a rare autosomal-dominant musculoskeletal disorder characterized by progressive heterotopic ossification. Ninety-seven percent of these patients carry an R206H gain-of-function point mutation in the bone morphogenetic protein (BMP) type I receptor ACVR1 (ACVR1R206H), which causes neofunction to Activin A and constitutively activates signaling through phosphorylated SMAD1/5/8. Although FOP patients can harbor pathological lesions in the peripheral and central nervous system, their etiology is unclear. Quantitative Sensory Testing (QST) of patients with FOP revealed significant heat and mechanical pain hypersensitivity. Although there was no major impact of ACVR1R206H on differentiation and maturation of nociceptive sensory neurons (iSNs) derived from FOP induced pluripotent stem cells (iPSCs), both intracellular and extracellular electrophysiology analysis of the ACVR1R206H iSNs displayed ACVR1-dependent hyperexcitability, a hallmark of neuropathic pain. Consistent with this phenotype, we recorded enhanced responses of ACVR1R206H iSNs to TRPV1 and TRPA1 agonists. Thus, activated ACVR1 signaling can modulate pain processing in humans and may represent a potential target for pain management in FOP and related BMP pathway diseases.

Published

2022

36. Understanding and modifying Fabry disease: Rationale and design of a pivotal Phase 3 study and results from a patient-reported outcome validation study

Author

Wanner, C, Wanner, C, Kimonis, V, Politei, J, Warnock, DG, Üçeyler, N, Frey, A, Cornelisse, P, Hughes, D, Wanner, C, Wanner, C, Kimonis, V, Politei, J, Warnock, DG, Üçeyler, N, Frey, A, Cornelisse, P, and Hughes, D

Abstract

The use of available treatments for Fabry disease (FD) (including enzyme replacement therapy [ERT]) may be restricted by their limited symptom improvement and mode of administration. Lucerastat is currently being investigated in the MODIFY study as oral substrate reduction therapy for the treatment of FD. By reducing the net globotriaosylceramide (Gb3) load in tissues, lucerastat has disease-modifying potential to improve symptoms and delay disease progression. MODIFY is a multicenter, double-blind, randomized, placebo-controlled, parallel-group Phase 3 study (ClinicalTrial.gov: NCT03425539); here we present the rationale and design of this study. Eligible adults with a genetically confirmed diagnosis of FD and FD-specific neuropathic pain entered screening. Patients were randomized (2:1) to receive either oral lucerastat twice daily or placebo for 6 months; treatment allocation was stratified according to sex and ERT treatment status. The main objectives of MODIFY are to assess the effects of lucerastat on neuropathic pain, gastrointestinal (GI) symptoms, FD biomarkers, and determine its safety and tolerability. Neuropathic pain and GI symptoms are key features of FD that have a significant impact on quality of life. Despite various tools available to assess pain and GI symptoms, there are currently limited tools available to assess neuropathic and GI symptoms in FD, validated according to health authority guidelines. Based on FDA recommendations, we undertook a patient-reported outcome (PRO) validation study, using a novel eDiary-based PRO tool to assess the validity of evaluating neuropathic pain as a primary efficacy endpoint in MODIFY. Results from the PRO validation study are included. To date, MODIFY is the largest Phase 3 clinical study conducted in patients with FD. Enrollment to MODIFY is now complete, with 118 patients randomized. Results will be presented in a separate publication. Long-term effects of lucerastat are being assessed in the ongoing open-la

Published

2022

37. Towards a better understanding of diabetic neuropathies in hands: A comprehensive assessment of nerve function, structure and mechanical properties

Author

Sierra Silvestre, Eva and Sierra Silvestre, Eva

Abstract

Distal symmetrical polyneuropathy (DSPN) is the most common complication in diabetes but little is known about how diabetes affects the nerves that supply the hands or why some people with DSPN develop neuropathic pain. This thesis assessed the structure, function, and mechanical properties of peripheral nerves using non-invasive methods in healthy individuals (n=31), people with diabetes without DSPN (n=35), with DSPN in feet only (n=31), and with DSPN in hands and feet (n=28). Quantitative sensory tests showed that people with DSPN presented with severe loss of nerve function in their hands, even if DSPN symptoms were only present in the feet. Diffusion MRI analyses showed microstructural changes in the nerves supplying the hands in people with DSPN in hands, in people with DSPN in feet, and in people with diabetes without DSPN. Shear-wave elastography revealed increased nerve stiffness. Regarding neuropathic pain in DSPN, our systematic review and meta-analysis showed a reduction in painful detection thresholds in people with non-painful and painful DSPN. Corneal confocal microscopy showed progressive nerve fibre loss across groups. The proportion of people with abnormal corneal epithelial microneuromas and their prevalence increased in people with painful DSPN compared to all other groups, including non-painful DSPN. Our findings suggest a potential progression of structural, functional, and mechanical changes in peripheral nerves supplying the hands as diabetes and DSPN progress.

Published

2022

38. Tremors in CIDP: A Wrist Perturbation Study

Author

Radhamohan Menon, Akshay (author) and Radhamohan Menon, Akshay (author)

Abstract

Chronic inflammatory demyelinating polyneuropathy (CIDP) is characterized by sensory and motor deficits. Tremor is a frequent and severe symptom in patients suffering from CIDP. There is limited and contradictory data regarding the effect of tremor on treatment of the underlying polyneuropathy, and on treatment specifically aimed at neuropathic tremor. The pathophysiology of the CIDP tremor is unknown, but there are speculations about both a peripheral and central origin. From previous studies, it is seen that if a tremor’s frequency is substantially load-independent, entrained exclusively by comparable driving frequencies, and only minimally phase-reset by torque pulses, it is considered to be primarily of central origin. A wrist perturbation study using a wrist manipulator was conducted on CIDP patients, with tremors (n=8) and without tremors (control, n=8) to address these speculations, and to understand the characteristics of this neuropathic tremor. The perturbation study involved studying the effects of entrainment perturbations, spring loading via changing the virtual spring stiffness, ramp-and-hold stretches to evoke stretch reflexes, along with the estimation of admittance. The entrainment task showed subharmonic and superharmonic peaks of power spectral densities of EMG in tremor subjects. Compared to controls, the tremor patients had significantly reduced stiffness, which could be attributed by the loss of muscle strength, and thus the tremor advertently affects muscle activation. No significant difference in M1, and M2 amplitude responses, and reflex latencies were found between the tremor and control group., Mechanical Engineering

Published

2022

39. Swedish Mutant Nerve Growth Factor (NGFR100W): Potential Therapeutic for Neurodegenerative Diseases

Author

Woo, Sangwon, Wu, Chengbiao1, Woo, Sangwon, Woo, Sangwon, Wu, Chengbiao1, and Woo, Sangwon

Abstract

Neurodegenerative diseases are characterized by loss of sensory neurons leading to motor, cognitive, and memory deficits. Due to the lack of a cure for such diseases, these diseases are costly in the United States. Extensive studies in the past showed the potential of nerve growth factor (NGF) as a therapeutic measure due to its trophic capabilities affecting the proliferation and regeneration of neurons. Therefore, NGF has been tried in several clinical trials, but all failed because of painful side effects such as site injection hyperalgesia or myalgia. However, the recent discovery of a mutant NGF (NGFR100W) that does not induce pain allowed us to investigate its potential as an alternative. Due to the blood-brain barrier limiting the administration of these NGF, we explored the effect of NGFR100W by injecting it into CharcotMarie Tooth Type 2B mouse models as they closely resemble peripheral neuropathy. We performed a hot plate test for nociception and sensitivity of the peripheral nerves by injecting increasing doses of NGFR100W. NGFR100W injected groups did not show significant pain perception compared to wild-type NGF injected groups even in high doses. Our immunohistochemistry data further indicated that NGFR100W prompted neuronal recovery comparable to that observed in wild-type NGF. We also explored the regenerative aspect of NGFR100W which rescued the sensory perception of the CMT2B mouse. Based on these findings, we validated the capability of NGFR100W in regenerating neurons and sensory function, which can be potentially used to improve the condition of individuals with peripheral neuropathy.

Published

2022

40. Proposed Linezolid Dosing Strategies to Minimize Adverse Events for Treatment of Extensively Drug-Resistant Tuberculosis.

Author

Imperial, Marjorie Z, Imperial, Marjorie Z, Nedelman, Jerry R, Conradie, Francesca, Savic, RM, Imperial, Marjorie Z, Imperial, Marjorie Z, Nedelman, Jerry R, Conradie, Francesca, and Savic, RM

Abstract

BackgroundWe evaluated Nix-TB trial data (NCT02333799, N = 109) to provide dosing recommendations to potentially minimize linezolid toxicity in patients with extensively drug-resistant tuberculosis. .MethodsA pharmacokinetic model and toxicodynamic models for peripheral neuropathy, hemoglobin, and platelets were developed. Simulations compared safety outcomes for daily linezolid of 1200 and 600 mg, with and without dose adjustments for toxicity. Severe neuropathy was based on symptom scores from the Brief Peripheral Neuropathy Screen. Severe anemia and thrombocytopenia were defined as ≥ grade 3 adverse events according to the NIAID Division of Microbiology and Infectious Disease Adult Toxicity table.ResultsPredicted concentration-time profiles were a major predictor in all toxicodynamic models. Simulations showed higher percentages of patients with severe neuropathy (median, 19%; 90% confidence interval [CI], 17%-22% vs 5%, 4%-7%) and severe anemia (15%, 12%-17% vs 1%, 0%-2%) between 1200 and 600 mg daily linezolid. No differences in severe thrombocytopenia were observed (median, <1% for both daily doses). Generally, neuropathy occurred after 3 to 6 months of treatment and, with protocol-specified management, reversed within 15 months after onset. Simulations indicated that a >10% decrease in hemoglobin level after 4 weeks of treatment would have maximum sensitivity (82%) and specificity (84%) for predicting severe anemia. Reducing the dose from 1200 to 600 mg triggered by this marker may prevent 60% (90% CI, 45%-72%) of severe anemia.ConclusionsSimple neuropathy symptom and hemoglobin monitoring may guide linezolid dosing to avoid toxicities, but prospective testing is needed to confirm the benefit-to-risk ratio.

Published

2022

41. Toward Composite Pain Biomarkers of Neuropathic Pain-Focus on Peripheral Neuropathic Pain.

Author

Diaz, Monica M, Diaz, Monica M, Caylor, Jacob, Strigo, Irina, Lerman, Imanuel, Henry, Brook, Lopez, Eduardo, Wallace, Mark S, Ellis, Ronald J, Simmons, Alan N, Keltner, John R, Diaz, Monica M, Diaz, Monica M, Caylor, Jacob, Strigo, Irina, Lerman, Imanuel, Henry, Brook, Lopez, Eduardo, Wallace, Mark S, Ellis, Ronald J, Simmons, Alan N, and Keltner, John R

Abstract

Chronic pain affects ~10-20% of the U.S. population with an estimated annual cost of $600 billion, the most significant economic cost of any disease to-date. Neuropathic pain is a type of chronic pain that is particularly difficult to manage and leads to significant disability and poor quality of life. Pain biomarkers offer the possibility to develop objective pain-related indicators that may help diagnose, treat, and improve the understanding of neuropathic pain pathophysiology. We review neuropathic pain mechanisms related to opiates, inflammation, and endocannabinoids with the objective of identifying composite biomarkers of neuropathic pain. In the literature, pain biomarkers typically are divided into physiological non-imaging pain biomarkers and brain imaging pain biomarkers. We review both types of biomarker types with the goal of identifying composite pain biomarkers that may improve recognition and treatment of neuropathic pain.

Published

2022

42. Intra-axonal translation of Khsrp mRNA slows axon regeneration by destabilizing localized mRNAs.

Author

Patel, Priyanka, Patel, Priyanka, Buchanan, Courtney N, Zdradzinski, Matthew D, Sahoo, Pabitra K, Kar, Amar N, Lee, Seung Joon, Vaughn, Lauren S, Urisman, Anatoly, Oses-Prieto, Juan, Dell'Orco, Michela, Cassidy, Devon E, Costa, Irene Dalla, Miller, Sharmina, Thames, Elizabeth, Smith, Terika P, Burlingame, Alma L, Perrone-Bizzozero, Nora, Twiss, Jeffery L, Patel, Priyanka, Patel, Priyanka, Buchanan, Courtney N, Zdradzinski, Matthew D, Sahoo, Pabitra K, Kar, Amar N, Lee, Seung Joon, Vaughn, Lauren S, Urisman, Anatoly, Oses-Prieto, Juan, Dell'Orco, Michela, Cassidy, Devon E, Costa, Irene Dalla, Miller, Sharmina, Thames, Elizabeth, Smith, Terika P, Burlingame, Alma L, Perrone-Bizzozero, Nora, and Twiss, Jeffery L

Abstract

Axonally synthesized proteins support nerve regeneration through retrograde signaling and local growth mechanisms. RNA binding proteins (RBP) are needed for this and other aspects of post-transcriptional regulation of neuronal mRNAs, but only a limited number of axonal RBPs are known. We used targeted proteomics to profile RBPs in peripheral nerve axons. We detected 76 proteins with reported RNA binding activity in axoplasm, and levels of several change with axon injury and regeneration. RBPs with altered levels include KHSRP that decreases neurite outgrowth in developing CNS neurons. Axonal KHSRP levels rapidly increase after injury remaining elevated up to 28 days post axotomy. Khsrp mRNA localizes into axons and the rapid increase in axonal KHSRP is through local translation of Khsrp mRNA in axons. KHSRP can bind to mRNAs with 3'UTR AU-rich elements and targets those transcripts to the cytoplasmic exosome for degradation. KHSRP knockout mice show increased axonal levels of KHSRP target mRNAs, Gap43, Snap25, and Fubp1, following sciatic nerve injury and these mice show accelerated nerve regeneration in vivo. Together, our data indicate that axonal translation of the RNA binding protein Khsrp mRNA following nerve injury serves to promote decay of other axonal mRNAs and slow axon regeneration.

Published

2022

43. In Vitro, In Vivo and Ex Vivo Models for Peripheral Nerve Injury and Regeneration.

Author

Li, Andrew, Li, Andrew, Pereira, Clifford, Hill, Elise Eleanor, Vukcevich, Olivia, Wang, Aijun, Li, Andrew, Li, Andrew, Pereira, Clifford, Hill, Elise Eleanor, Vukcevich, Olivia, and Wang, Aijun

Abstract

Peripheral Nerve Injuries (PNI) frequently occur secondary to traumatic injuries. Recovery from these injuries can be expectedly poor, especially in proximal injuries. In order to study and improve peripheral nerve regeneration, scientists rely on peripheral nerve models to identify and test therapeutic interventions. In this review, we discuss the best described and most commonly used peripheral nerve models that scientists have and continue to use to study peripheral nerve physiology and function.

Published

2022

44. Simultaneous monitoring of mouse grip strength, force profile, and cumulative force profile distinguishes muscle physiology following surgical, pharmacologic and diet interventions.

Author

Munier, Joseph J, Munier, Joseph J, Pank, Justin T, Severino, Amie, Wang, Huan, Zhang, Peixiang, Vergnes, Laurent, Reue, Karen, Munier, Joseph J, Munier, Joseph J, Pank, Justin T, Severino, Amie, Wang, Huan, Zhang, Peixiang, Vergnes, Laurent, and Reue, Karen

Abstract

Grip strength is a valuable preclinical assay to study muscle physiology in disease and aging by directly determining changes in muscle force generation in active laboratory mice. Existing methods to statistically evaluate grip strength, however, have limitations in the power and scope of the physiological features that are assessed. We therefore designed a microcontroller whose serial measure of resistance-based force enables the simultaneous readout of (1) peak grip strength, (2) force profile (the non-linear progress of force exerted throughout a standard grip strength trial), and (3) cumulative force profile (the integral of force with respect to time of a single grip strength trial). We hypothesized that muscle pathologies of different etiologies have distinct effects on these parameters. To test this, we used our apparatus to assess the three muscle parameters in mice with impaired muscle function resulting from surgically induced peripheral pain, genetic peripheral neuropathy, adverse muscle effects induced by statin drug, and metabolic alterations induced by a high-fat diet. Both surgically induced peripheral nerve injury and statin-associated muscle damage diminished grip strength and force profile, without affecting cumulative force profile. Conversely, genetic peripheral neuropathy resulting from lipin 1 deficiency led to a marked reduction to all three parameters. A chronic high-fat diet led to reduced grip strength and force profile when normalized to body weight. In high-fat fed mice that were exerted aerobically and allowed to recover for 30 min, male mice exhibited impaired force profile parameters, which female mice were more resilient. Thus, simultaneous analysis of peak grip strength, force profile and cumulative force profile distinguishes the muscle impairments that result from distinct perturbations and may reflect distinct motor unit recruitment strategies.

Published

2022

45. Alterations in brain structure associated with trigeminal nerve anatomy in episodic migraine.

Author

Mungoven, Tiffani J, Mungoven, Tiffani J, Meylakh, Noemi, Macefield, Vaughan G, Macey, Paul M, Henderson, Luke A, Mungoven, Tiffani J, Mungoven, Tiffani J, Meylakh, Noemi, Macefield, Vaughan G, Macey, Paul M, and Henderson, Luke A

Abstract

The pathophysiology of migraine remains to be elucidated. We have recently shown that interictal migraineurs exhibit reduced fractional anisotropy (FA) in the root entry zone of the trigeminal nerve when compared to controls, but it is not known if this altered nerve anatomy is associated with changes within the brainstem or higher cortical brain regions. Diffusion tensor imaging of the brain was used to calculate regional measures of structure, including mean diffusivity (MD), axial diffusivity (AX) and radial diffusivity (RD) in addition to voxel-based morphometry of T1-weighted anatomical images. Linear relationships between trigeminal nerve anatomy (FA) and MD throughout the brainstem and/or higher cortical regions were determined in both controls (n = 31, brainstem; n = 38, wholebrain) and interictal migraineurs (n = 32, brainstem; n = 38, wholebrain). Additionally, within the same brain areas, relationships of AX and RD with nerve FA were determined. We found that in both interictal migraine and control participants, decreasing trigeminal nerve FA was associated with significantly increased MD in brainstem regions including the spinal trigeminal nucleus and midbrain periaqueductal gray matter (PAG), and in higher brain regions such as the hypothalamus, insula, posterior cingulate, primary somatosensory and primary visual (V1) cortices. Whereas, both control and migraineur groups individually displayed significant inverse correlations between nerve FA and MD, in migraineurs this pattern was disrupted in the areas of the PAG and V1, with only the control group displaying a significant linear relationship (PAG controls r = -0.58, p = 0.003; migraineurs r = -0.25, p = 0.17 and V1 controls r = -0.52, p = 0.002; migraineurs r = -0.10, p = 0.55). Contrastingly, we found no gray matter volume changes in brainstem or wholebrain areas. These data show that overall, trigeminal nerve anatomy is significantly related to regional brain structure in both controls and migrain

Published

2022

46. Blockade of dopamine D1 receptors in male rats disrupts morphine reward in pain naïve but not in chronic pain states.

Author

Grenier, Patrick, Grenier, Patrick, Mailhiot, Madison C, Cahill, Catherine M, Olmstead, Mary C, Grenier, Patrick, Grenier, Patrick, Mailhiot, Madison C, Cahill, Catherine M, and Olmstead, Mary C

Abstract

The rewarding effect of opiates is mediated through dissociable neural systems in drug naïve and drug-dependent states. Neuroadaptations associated with chronic drug use are similar to those produced by chronic pain, suggesting that opiate reward could also involve distinct mechanisms in chronic pain and pain-naïve states. We tested this hypothesis by examining the effect of dopamine (DA) antagonism on morphine reward in a rat model of neuropathic pain.Neuropathic pain was induced in male Sprague-Dawley rats through chronic constriction (CCI) of the sciatic nerve; reward was assessed in the conditioned place preference (CPP) paradigm in separate groups at early (4-8 days post-surgery) and late (11-15 days post-surgery) phases of neuropathic pain. Minimal effective doses of morphine that produced a CPP in early and late phases of neuropathic pain were 6 mg/kg and 2 mg/kg respectively. The DA D1 receptor antagonist, SCH23390, blocked a morphine CPP in sham, but not CCI, rats at a higher dose (0.5 mg/kg), but had no effect at a lower dose (0.1 mg/kg). The DA D2 receptor antagonist, eticlopride (0.1 and 0.5 mg/kg), had no effect on a morphine CPP in sham or CCI rats, either in early or late phases of neuropathic pain. In the CPP paradigm, morphine reward involves DA D1 mechanisms in pain-naïve but not chronic pain states. This could reflect increased sensitivity to drug effects in pain versus no pain conditions and/or differential mediation of opiate reward in these two states.

Published

2022

47. OBITUARY Maarten van Kleef, MD, PhD-1953-2022

Author

Van Zundert, J., Van Zundert, J., Liem, L., Joosten, B., Van Zundert, J., Van Zundert, J., Liem, L., and Joosten, B.

Published

2022

48. Peripheral neuropathy:A neglected cause of disability in COPD – A narrative review

Author

Odajiu, Irina, Covantsev, Serghei, Sivapalan, Pradeesh, Mathioudakis, Alexander G., Jensen, Jens Ulrik Stæhr, Davidescu, Eugenia Irene, Chatzimavridou-Grigoriadou, Victoria, Corlateanu, Alexandru, Odajiu, Irina, Covantsev, Serghei, Sivapalan, Pradeesh, Mathioudakis, Alexander G., Jensen, Jens Ulrik Stæhr, Davidescu, Eugenia Irene, Chatzimavridou-Grigoriadou, Victoria, and Corlateanu, Alexandru

Abstract

Chronic obstructive pulmonary disease (COPD) is a chronic inflammatory syndrome with systemic involvement leading to various cardiovascular, metabolic, and neurological comorbidities. It is well known that conditions associated with oxygen deprivation and metabolic disturbance are associated with polyneuropathy, but current data regarding the relationship between COPD and peripheral nervous system pathology is limited. This review summarizes the available data on the association between COPD and polyneuropathy, including possible pathophysiological mechanisms such as the role of hypoxia, proinflammatory state, and smoking in nerve damage; the role of cardiovascular and metabolic comorbidities, as well as the diagnostic methods and screening tools for identifying polyneuropathy. Furthermore, it outlines the available options for managing and preventing polyneuropathy in COPD patients. Overall, current data suggest that optimal screening strategies to diagnose polyneuropathy early should be implemented in COPD patients due to their relatively common association and the additional burden of polyneuropathy on quality of life.

Published

2022

49. Vitamin B 12 Levels in Patients with Type 2 Diabetes Mellitus on Metformin

Author

V Padma, NN Anand, V Padma, and NN Anand

Abstract

Vitamin B12 is required for proper hematopoeisis, cardiovascular and neurocognitive function. Vitamin B12 deficiency is highly prevalent among patients with type 2 diabetes mellitus (T2DM) on metformin therapy. Aim: This study was carried out to evaluate the serum levels of vitamin B12 in patients with T2DM on metformin therapy. Material and methods: Hundred patients with T2DM within the age group of 45-80 years were recruited into this cross-sectional study. All the patients were on metformin therapy for a minimum of 5 years. Results: Vitamin B12 deficiency and borderline deficiency observed were 10.6% and 29% and 60.4% did not have vitamin B12 deficiency. B12 levels were lower in patients with more than 10 years of duration of diabetes and was statistically significant with a p value of 0.004. The average B12 levels in patients on metformin dose of >1,000 mg was 349 pg/dL and in patients with metformin dose above 1,000 mg was 215 pg/dL. The difference between the two groups was statistically significant with a p value of <0.002. Conclusion: There is a high prevalence of B 12 deficiency among diabetic patients. It is important to screen for vitamin B12 deficiency before initiating metformin and later annually.

Published

2022

50. Cisplatin Neurotoxicity Targets Specific Subpopulations and K+ Channels in Tyrosine-Hydroxylase Positive Dorsal Root Ganglia Neurons.

Author

Finno, Carrie J, Finno, Carrie J, Chen, Yingying, Park, Seojin, Lee, Jeong Han, Perez-Flores, Maria Cristina, Choi, Jinsil, Yamoah, Ebenezer N, Finno, Carrie J, Finno, Carrie J, Chen, Yingying, Park, Seojin, Lee, Jeong Han, Perez-Flores, Maria Cristina, Choi, Jinsil, and Yamoah, Ebenezer N

Abstract

Among the features of cisplatin chemotherapy-induced peripheral neuropathy are chronic pain and innocuous mechanical hypersensitivity. The complete etiology of the latter remains unknown. Here, we show that cisplatin targets a heterogeneous population of tyrosine hydroxylase-positive (TH+) primary afferent dorsal root ganglion neurons (DRGNs) in mice, determined using single-cell transcriptome and electrophysiological analyses. TH+ DRGNs regulate innocuous mechanical sensation through C-low threshold mechanoreceptors. A differential assessment of wild-type and vitamin E deficient TH+ DRGNs revealed heterogeneity and specific functional phenotypes. The TH+ DRGNs comprise; fast-adapting eliciting one action potential (AP; 1-AP), moderately-adapting (≥2-APs), in responses to square-pulse current injection, and spontaneously active (SA). Cisplatin increased the input resistance and AP frequency but reduced the temporal coding feature of 1-AP and ≥2-APs neurons. By contrast, cisplatin has no measurable effect on the SA neurons. Vitamin E reduced the cisplatin-mediated increased excitability but did not improve the TH+ neuron temporal coding properties. Cisplatin mediates its effect by targeting outward K+ current, likely carried through K2P18.1 (Kcnk18), discovered through the differential transcriptome studies and heterologous expression. Studies show a potential new cellular target for chemotherapy-induced peripheral neuropathy and implicate the possible neuroprotective effects of vitamin E in cisplatin chemotherapy.

Published

2022