Saif Muhammad Wasif, Peccerillo J, Potter Von
Section of Medical Oncology, Yale University School of Medicine, 333 Cedar Street, FMP 116, New Haven, CT 06520, USA.
Cancer Chemother Pharmacol. 2009 May;63(6):1017-22. doi: 10.1007/s00280-008-0831-6. Epub 2008 Sep 10.
Monoclonal antibodies (MAbs) targeting epidermal growth factor receptor (EGFR) are effective in treatment of metastatic colorectal cancer (mCRC). Cetuximab, a chimeric MAb targets EGFR. Even with premedication, cetuximab can cause a hypersensitivity reaction (HSR). In case of severe HSR, further therapy with cetuximab is contraindicated, thus preventing these patients from receiving potentially beneficial anti-EGFR therapy. Panitumumab is a fully human MAb also targets EGFR. To date, no human antihuman Ab have been detected, and unlike CET, HSR are infrequent, and no premedication is required. Safety of panitumumab in patients with a previous severe HSR with cetuximab is not fully known. We present three patients with GI cancers who tolerated panitumumab without HSR after experiencing severe HSR to cetuximab.
Three patients were challenged with standard dose of panitumumab (6 mg/kg) after experiencing grade 3 HSR to standard dose of cetuximab under strict observation and no premedication. First patient, a 58-year-old male with mCRC developed grade 3 HSR during 8th dose of cetuximab. Second patient was a 58-year-old female with mCRC developed grade 3 HSR during 12th dose of cetuximab. Third patient was a 61-year-old male with pancreatic cancer who experienced grade 3 HSR during loading dose of cetuximab. Charts were reviewed to find history of prior allergy, including H1 blocker use, drug allergy, bee sting allergy, eczema, allergic reactive airways disease, or food allergy.
All patients were Caucasians with an average age of 59 year with no history of prior allergy. No patient received any premedication. First patient received panitumumab for 2 months, second patient was treated for 6 months, and third patient who was rechallenged 1 week after HSR to cetuximab had a partial response following 6 months of therapy.
HSR are serious complications associated with MAbs. Thanks to hybridoma technology that newer generations of MAbs contain less or no mouse-specific protein sequences, hence reducing the risk of HSR. Identification of individuals likely to develop severe and sometimes life-threatening HSR is challenging. Our report of three patients successfully treated with panitumumab after they had severe HSR to cetuximab warrant further investigation.
靶向表皮生长因子受体(EGFR)的单克隆抗体(MAb)在转移性结直肠癌(mCRC)治疗中有效。西妥昔单抗是一种靶向EGFR的嵌合单克隆抗体。即使进行了预处理,西妥昔单抗仍可引起过敏反应(HSR)。在严重HSR的情况下,禁忌使用西妥昔单抗进行进一步治疗,从而使这些患者无法接受可能有益的抗EGFR治疗。帕尼单抗是一种同样靶向EGFR的全人源单克隆抗体。迄今为止,尚未检测到人类抗人抗体,与西妥昔单抗不同,HSR很少见,且无需预处理。帕尼单抗在先前使用西妥昔单抗发生严重HSR的患者中的安全性尚不完全清楚。我们报告了3例胃肠道癌症患者,他们在对西妥昔单抗发生严重HSR后耐受了帕尼单抗且未发生HSR。
3例患者在严格观察且未进行预处理的情况下,在对标准剂量西妥昔单抗发生3级HSR后,接受标准剂量帕尼单抗(6mg/kg)激发试验。首例患者为一名58岁男性mCRC患者,在第8剂西妥昔单抗治疗期间发生3级HSR。第二例患者为一名58岁女性mCRC患者,在第12剂西妥昔单抗治疗期间发生3级HSR。第三例患者为一名61岁男性胰腺癌患者,在西妥昔单抗负荷剂量治疗期间发生3级HSR。查阅病历以查找既往过敏史,包括使用H1阻滞剂、药物过敏、蜂蜇过敏、湿疹、过敏性反应性气道疾病或食物过敏史。
所有患者均为白种人,平均年龄59岁,无既往过敏史。无患者接受任何预处理。首例患者接受帕尼单抗治疗2个月,第二例患者接受治疗6个月,第三例患者在对西妥昔单抗发生HSR后1周再次接受激发试验,治疗6个月后出现部分缓解。
HSR是与单克隆抗体相关的严重并发症。得益于杂交瘤技术,新一代单克隆抗体含较少或不含小鼠特异性蛋白序列,从而降低了HSR风险。识别可能发生严重且有时危及生命的HSR的个体具有挑战性。我们报告的3例患者在对西妥昔单抗发生严重HSR后成功接受帕尼单抗治疗,值得进一步研究。
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