Early Complications of High-Dose Methylprednisolone Sodium Succinate Treatment in the Follow-Up of Acute Cervical Spinal Cord Injury

Matsumoto, Taihei; Tamaki, Toru; Kawakami, Mamoru; Yoshida, Munehito; Ando, Muneharu; Yamada, Hiroshi

doi:10.1097/00007632-200102150-00020

Cited by 194 publications

(114 citation statements)

References 15 publications

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“…In particular, the incidence of wound infection, sepsis, pneumonia, and the duration of intensive care unit stay have all been increased in patients receiving high-dose methylprednisolone. 13,15,20,[46][47][48][49] Intravenous methylprednisolone must be administered in such high doses because, as we have previously shown, methylprednisolone entry into the central nervous system is actively opposed by P-glycoprotein present in the capillary endothelial cells comprising the brain-and spinal cord-blood barriers. 50 As P-glycoprotein actively pumps methylprednisolone out of the central nervous system, systemically administered methylprednisolone must be given in very high doses to overwhelm the efflux pump's capacity and to achieve reasonable concentrations in the central nervous system.…”

Section: Discussionmentioning

confidence: 99%

Effect of postinjury intravenous or intrathecal methylprednisolone on spinal cord excitatory amino-acid release, nitric oxide generation, PGE2 synthesis, and myeloperoxidase content in a pig model of acute spinal cord injury

Bernards

Akers

2006

Spinal Cord

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Objectives: To determine whether postinjury methylprednisolone could reduce the generation of known mediators of secondary neurological injury. Methods: Intrathecal microdialysis probes were used to sample cerebrospinal fluid (CSF) for measurement of PGE 2 , glutamate, and citrulline (a byproduct of nitric oxide generation), before and after spinal cord injury in anesthetized pigs. The spinal cord was removed at the end of the study for measurement of myeloperoxidase and methylprednisolone concentrations. Animals were randomly allocated to receive intravenous methylprednisolone (30 mg/kg bolus then 3.4 mg/kg/h), intrathecal methylprednisolone (5 mg bolus then 5 mg/h), or saline, beginning 30 min after the spinal cord was injured by using a modification of the Allen weight drop technique. Results: Spinal cord injury significantly increased the amount of glutamate, PGE 2 , myeloperoxidase, and citrulline, recovered from the CSF dialysates. However, neither intravenous nor intrathecal methylprednisolone administered after injury had any effect on the magnitude of the increase in any of the measured biochemicals. Intrathecal methylprednisolone administration produced a spinal cord methylprednisolone concentration that was eight times greater, and a plasma concentration that was 32 times less, than that achieved with intravenous administration. Conclusions: Contrary to earlier animal studies in which methylprednisolone was administered either before or immediately after spinal cord injury, we found no effect of intravenous or intrathecal methylprednisolone on any of the parameters measured when administered 30 min postinjury.

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Section: Discussionmentioning

confidence: 99%

Effect of postinjury intravenous or intrathecal methylprednisolone on spinal cord excitatory amino-acid release, nitric oxide generation, PGE2 synthesis, and myeloperoxidase content in a pig model of acute spinal cord injury

Bernards

Akers

2006

Spinal Cord

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“…After this study, the use of intravenous high-dose methylprednisolone became a standard approach in acute management of SCI patients (47). However, two other studies reported that high-dose methylprednisolone could be associated increased complication rates (48,49).…”

Section: Steroids In Spinal Cord Injurymentioning

confidence: 99%

Acute Management of Spinal Cord Injury at the Out-of-Hospital and Emergency Department Settings

Katipoğlu¹,

Dagal²,

Korkut³

et al. 2017

EAJEM

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“…16,17 At the same time, the safety of MP treatment was being challenged by the publication of a number of non-randomized case series reports, suggesting an association between treatment and immune system compromise, pneumonia, mechanical ventilation days, gastrointestinal complications and myopathy. [18][19][20][21] The Great Debate: the quality of NASCIS evidence While the debate over the validity of NASCIS 2 and 3 conclusions may have been motivated by many factors including timing of the public dissemination, and feelings that a far-reaching standard had been imposed without proper vetting, the substance of the argument revolved around the quality of the evidence. While a thorough review of the various positions is well beyond the scope of this communication, the interested reader is encouraged to consult the abundant literature on the topic that has been published over the past 20 years.…”

Section: The Methylprednisolone Story Nascis 1: Prevailing Dogma Is Omentioning

confidence: 99%

Clinical trials in spinal cord injury: lessons learned on the path to translation. The 2011 International Spinal Cord Society Sir Ludwig Guttmann Lecture

Lammertse

2012

Spinal Cord

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After three decades of clinical research on interventions to improve neurological outcomes in persons with spinal cord injury (SCI), the promise of preclinical discovery has yet to be translated into a consensus standard of care treatment. Nonetheless, SCI researchers remain hopeful that advances in preclinical discovery coupled with improved clinical trial performance will yield effective restorative treatment. This historical review of key studies in SCI over the past 30 years illustrates the progress that has been achieved in establishing a high standard in the conduct of clinical research while providing important lessons for improving trial design, conduct and reporting. Through application of these lessons, the performance of SCI trials can be improved, thereby shortening the pathway to successful translation and the development of effective therapies.

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Early Complications of High-Dose Methylprednisolone Sodium Succinate Treatment in the Follow-Up of Acute Cervical Spinal Cord Injury

Abstract: Aged patients with cervical spinal injury may be more likely to have pulmonary side effects (P = 0.029) after high-dose therapy with MPSS and thus deserve special care.

Cited by 194 publications

References 15 publications

Effect of postinjury intravenous or intrathecal methylprednisolone on spinal cord excitatory amino-acid release, nitric oxide generation, PGE2 synthesis, and myeloperoxidase content in a pig model of acute spinal cord injury

Effect of postinjury intravenous or intrathecal methylprednisolone on spinal cord excitatory amino-acid release, nitric oxide generation, PGE2 synthesis, and myeloperoxidase content in a pig model of acute spinal cord injury

Acute Management of Spinal Cord Injury at the Out-of-Hospital and Emergency Department Settings

Clinical trials in spinal cord injury: lessons learned on the path to translation. The 2011 International Spinal Cord Society Sir Ludwig Guttmann Lecture

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