2016
DOI: 10.1002/art.39492
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When Is Osteonecrosis Not Osteonecrosis?: Adjudication of Reported Serious Adverse Joint Events in the Tanezumab Clinical Development Program

Abstract: Objective. Tanezumab, a monoclonal antibody against nerve growth factor, has demonstrated efficacy in clinical trials of chronic pain in osteoarthritis (OA) and chronic low back pain. Unexpected adverse events (AEs) described as osteonecrosis (ON) occurred during tanezumab development, leading the US Food and Drug Administration to impose a partial clinical hold for all indications except cancer pain. A blinded Adjudication Committee (AC) including orthopedic surgeons, rheumatologists, and an orthopedic pathol… Show more

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Cited by 136 publications
(151 citation statements)
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(56 reference statements)
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“…For example, Anti-NGF antibodies (tanezumab, fulranumab and fasinumab) have proven in a very unusual twist to be more efficacious in patients with osteoarthritis (OA) than the preclinical data would have expected 258 , with greater signals than gold standard NSAIDs and opioids for chronic low back pain – sometimes thought of as the graveyard of analgesic trials – as well as in OA and diabetic neuropathy 259261 . Conversely, tenezumab has been found to produce rapid progression of OA particularly when administered at high doses and with NSAIDs 262 . While the cause of this is uncertain, one possibility is that overuse of damaged joints because of high analgesia coverage may lead to accelerating joint destruction – pain is after all a protective mechanism as well as a disease burden.…”
Section: Challenges and Considerations In The Clinical Development Ofmentioning
confidence: 99%
“…For example, Anti-NGF antibodies (tanezumab, fulranumab and fasinumab) have proven in a very unusual twist to be more efficacious in patients with osteoarthritis (OA) than the preclinical data would have expected 258 , with greater signals than gold standard NSAIDs and opioids for chronic low back pain – sometimes thought of as the graveyard of analgesic trials – as well as in OA and diabetic neuropathy 259261 . Conversely, tenezumab has been found to produce rapid progression of OA particularly when administered at high doses and with NSAIDs 262 . While the cause of this is uncertain, one possibility is that overuse of damaged joints because of high analgesia coverage may lead to accelerating joint destruction – pain is after all a protective mechanism as well as a disease burden.…”
Section: Challenges and Considerations In The Clinical Development Ofmentioning
confidence: 99%
“…The adjudication committee could demonstrate unambiguous osteonecrosis in only two of the 86 reported osteonecrosis cases (although eight of those had insufficient information to distinguish primary osteonecrosis and the committee failed to reach consensus on another five) (20). …”
mentioning
confidence: 99%
“…Several pharmaceutical programs evaluating anti-nerve growth factor (a-NGF) compounds at present defined the atrophic OA phenotype as a potential risk factor for potential joint adverse events such as rapid progression or osteonecrosis 19,20 . Our data does not support this assumption, but it needs to be clearly acknowledged that subjects in the MOST study were not under a-NGF treatment and are thus not comparable to a-NGF cohorts.…”
Section: Discussionmentioning
confidence: 99%