2012
DOI: 10.1016/j.clcc.2011.10.004
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Literature Review and Practical Aspects on the Management of Oxaliplatin-Associated Toxicity

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Cited by 72 publications
(40 citation statements)
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“…Adding oxaliplatin to fluoropyrimidine chemotherapy results in increased grade 3 or 4 cytopenias and diarrhea, as well as both acute and chronic neurotoxicity. 2,4,6,7 In both NSABP C-07 and MOSAIC, peripheral neuropathy of any grade was observed in more than 60% of patients during oxaliplatin treatment, with 22% of patients reporting symptoms 18 months from random assignment in NSABP C-07 and 15% of patients reporting symptoms at 4 years in MOSAIC. 2,4 Recent studies focused on assessing the long-term consequences of oxaliplatin treatment suggest that chronic neurotoxicity is likely more prevalent than previously reported.…”
Section: 19mentioning
confidence: 99%
See 1 more Smart Citation
“…Adding oxaliplatin to fluoropyrimidine chemotherapy results in increased grade 3 or 4 cytopenias and diarrhea, as well as both acute and chronic neurotoxicity. 2,4,6,7 In both NSABP C-07 and MOSAIC, peripheral neuropathy of any grade was observed in more than 60% of patients during oxaliplatin treatment, with 22% of patients reporting symptoms 18 months from random assignment in NSABP C-07 and 15% of patients reporting symptoms at 4 years in MOSAIC. 2,4 Recent studies focused on assessing the long-term consequences of oxaliplatin treatment suggest that chronic neurotoxicity is likely more prevalent than previously reported.…”
Section: 19mentioning
confidence: 99%
“…Concerns over oxaliplatin-induced neuropathy have prompted multiple clinical trials evaluating interventions to mitigate this toxicity. 6,7 With a need to balance limited absolute benefit against significant toxicity, the prevailing paradigm has focused on directing adjuvant therapy to patients at higher recurrence risk, with the expectation of larger absolute treatment benefit. 8,9 Although stage does not predict for the relative benefit of fluorouracil (FU)/leucovorin (LV) or oxaliplatin, stage III patients, compared with stage II patients, have higher recurrence risk and larger absolute treatment benefit.…”
Section: Journal Of Clinical Oncology O R I G I N a L R E P O R T V Omentioning
confidence: 99%
“…The thirdgeneration platinum drug oxaliplatin is typically administered in a combination known as FOLFOX (with fluorouracil and leucovorin) for the treatment of advanced colorectal cancer. Oxaliplatin has less ototoxicity and nephrotoxicity than cisplatin but it can cause an acute painful neuropathy soon after administration (see Hoff et al, 2012), leading to paresthesias (which usually start periorally and then spread to the extremities) and severe cold hypersensitivity. Indeed, exposure to cold can trigger an acute, transient syndrome characterized by cramps, paresthesia, and dysesthesia in patients taking oxaliplatin, presumably by activating TRPA1 .…”
Section: Transient Receptor Potential Channels: Acquired Diseasesmentioning
confidence: 99%
“…These symptoms are rapidly reversible upon infusion discontinuation even in the absence of treatment (no need for antithistamines, corticoids or bronchodilators), and should be distinguished from hypersensitivity reactions. Other less common side effects include muscle spasms (often jaw spasms), balance disorders, throat or chest pressure/discomfort/pain, and cranial nerve dysfunctions (ptosis, diplopia, dysphonia, abnormal tongue sensation or dysarthria, visual disorders) [53,55] .…”
Section: Oxaliplatinmentioning
confidence: 99%