Jahraus Christopher D, Bettenhausen Doug, Malik Uzma, Sellitti Marguerite, St Clair William H
Department of Radiation Medicine, University of Kentucky College of Medicine, Lexington, KY, USA.
Int J Radiat Oncol Biol Phys. 2005 Dec 1;63(5):1483-7. doi: 10.1016/j.ijrobp.2005.04.032. Epub 2005 Aug 15.
A common complication of pelvic radiotherapy (RT) is acute radiation-induced proctosigmoiditis (RIPS), for which a multitude of therapies have been tried. The 5-aminosalicylates (5-ASA), which are traditionally used to treat inflammatory bowel disease, have been tested; however, all but one prior randomized attempt to limit or prevent RIPS with 5-ASA-type agents have failed. We sought to evaluate balsalazide, a new 5-ASA drug, for its potential to prevent or limit RIPS in patients undergoing RT for carcinoma of the prostate, as a representative sample of pelvic RT patients. Balsalazide has a unique delivery system in that 99% of ingested drug is delivered to and activated in the colon, a higher yield than all other oral agents currently available in this class. Furthermore, it lacks the antigenic sulfa moiety present in sulfasalazine, the only other 5-ASA with demonstrated benefit in this setting. Thus, it was deemed an ideal candidate for preventing or limiting RIPS.
Eligible patients included prostate cancer patients, American Joint Committee on Cancer Stage T1-3, M0 being treated with external beam radiotherapy in the University of Kentucky Department of Radiation Medicine. Between January 1, 2003 and July 1, 2004, 27 eligible patients were enrolled in the study. Patients were administered 2250 mg of balsalazide or an identical-appearing placebo twice daily beginning 5 days before RT and continuing for 2 weeks after completion. Toxicities were graded weekly according to National Cancer Institute Common Toxicity Criteria v. 2.0 for each of the following: proctitis, diarrhea, dysuria, weight loss, fatigue, nausea, and vomiting. A symptom index was formulated for each toxicity consisting of the toxicity's numeric grade multiplied by the number of days it was experienced, and summed for each grade experienced throughout the course of RT.
With the exception of nausea or vomiting, seen in 3 patients on balsalazide and 2 on placebo, all toxicities were appreciably lower in patients taking balsalazide. Proctitis was prevented most significantly with a mean proctitis index of 35.3 in balsalazide patients and 74.1 in placebo patients (p = 0.04). Placebo patients lost an average of 2.7 pounds, whereas balsalazide patients on average gained weight. Unexpectedly, dysuria was also lower in balsalazide-treated patients.
Balsalazide is a new-generation 5-ASA drug that yields a high concentration of active drug to the distal colon. Results of this pilot study suggest that it is able to prevent or reduce symptoms of RIPS in patients undergoing RT for prostate cancer. We feel that these results justify the formation of a cooperative group trial to assess its efficacy in a multi-institutional setting.
盆腔放疗(RT)的一种常见并发症是急性放射性直肠乙状结肠炎(RIPS),针对这一并发症人们尝试了多种治疗方法。传统上用于治疗炎症性肠病的5-氨基水杨酸酯(5-ASA)已接受过测试;然而,此前除一项随机试验外,所有试图用5-ASA类药物限制或预防RIPS的尝试均告失败。我们试图评估一种新型5-ASA药物巴柳氮,看其对于接受前列腺癌放疗的患者预防或限制RIPS的潜力,此类患者可作为盆腔放疗患者的代表性样本。巴柳氮具有独特的给药系统,即摄入药物的99%会被输送至结肠并在结肠内激活,这一转化率高于目前该类别中所有其他口服制剂。此外,它不像柳氮磺胺吡啶那样含有具有抗原性的磺胺部分,柳氮磺胺吡啶是在此种情况下唯一已证实有疗效的另一种5-ASA药物。因此,它被认为是预防或限制RIPS的理想候选药物。
符合条件的患者包括肯塔基大学放射医学系中接受外照射放疗的美国癌症联合委员会癌症分期为T1 - 3、M0的前列腺癌患者。在2003年1月1日至2004年7月1日期间,27名符合条件的患者被纳入该研究。患者从放疗前5天开始,每天两次服用2250毫克巴柳氮或外观相同的安慰剂,并在放疗结束后持续服用2周。根据美国国立癌症研究所通用毒性标准第2.0版,每周对以下各项毒性进行分级:直肠炎、腹泻、排尿困难、体重减轻、疲劳、恶心和呕吐。针对每种毒性制定一个症状指数,该指数由毒性的数字分级乘以出现该毒性的天数得出,并对放疗过程中出现的每个分级进行求和。
除了在服用巴柳氮的3名患者和服用安慰剂的2名患者中出现的恶心或呕吐外,服用巴柳氮的患者所有其他毒性均明显较低。巴柳氮对直肠炎的预防效果最为显著,服用巴柳氮患者的直肠炎平均指数为35.3,服用安慰剂患者的直肠炎平均指数为74.1(p = 0.04)。服用安慰剂的患者平均体重减轻2.7磅,而服用巴柳氮的患者平均体重增加。出乎意料的是,接受巴柳氮治疗的患者排尿困难情况也较少。
巴柳氮是一种新一代5-ASA药物,能在远端结肠产生高浓度的活性药物。这项初步研究结果表明,它能够预防或减轻接受前列腺癌放疗患者的RIPS症状。我们认为这些结果为开展一项合作组试验以评估其在多机构环境中的疗效提供了依据。
