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影响癌胚抗原表达肿瘤的放射免疫检测及放射免疫治疗的药代动力学、剂量测定和诊断准确性的因素。

Factors influencing the pharmacokinetics, dosimetry, and diagnostic accuracy of radioimmunodetection and radioimmunotherapy of carcinoembryonic antigen-expressing tumors.

作者信息

Behr T M, Sharkey R M, Juweid M I, Dunn R M, Ying Z, Zhang C H, Siegel J A, Gold D V, Goldenberg D M

机构信息

Garden State Cancer Center at the Center for Molecular Medicine and Immunology, Newark, New Jersey 07103, USA.

出版信息

Cancer Res. 1996 Apr 15;56(8):1805-16.

PMID:8620497
Abstract

The aim of this study was to examine factors that may influence the pharmacokinetics, diagnostic accuracy, and dosimetry in radioimmunodetection and radioimmunotherapy with anti-carcinoembryonic antigen (CEA) monoclonal antibodies (mAbs). Data from 275 patients with CEA expressing tumors were analyzed retrospectively. Of these, 69 patients devoid of human antimouse antibody (i.e., 31 colorectal, 9 lung, 7 breast, 4 ovarian, 6 pancreatic, 9 medullary thyroid, 1 gallbladder, and 1 salivary gland cancer, and 1 primary tumor of unknown origin) underwent a low-protein-dose diagnostic study (0.3-2.6 mg of protein; 6.8-28.8 mCi 131I-labeled IgG or fragments), followed within 4 weeks by a high-protein-dose therapy injection (4.0-27.5 mg of protein; 29.8-238.9 mCi). The anti-CEA antibodies NP-4 (Ka=10(8)M-1) and MN-14 (ka=10(9)M-1) were used. Plasma clearance, the molecular composition of radioactivity in the plasma, and the cumulated activity in organs and tumors were determined. Radiation doses were derived from the Medical Internal Radiation Dose scheme. At a low-protein dose and over a similar range of plasma CEA, a significantly higher percentage of MN-14 than of NP-4 was complexed with circulating CEA, consistent with its higher affinity. Complexation was reduced with increasing protein doses. However, the targeting sensitivity was not affected. Profound differences were found in the clearance of the antibody between different types of cancer. Colorectal cancer patients cleared the antibody significantly faster from blood (T1/2=17.6+/-12.6 versus 44.2 +/- 23.7 h) and whole body (t1/2= 53.2 +/- 30.1 versus 114.6+/-59.7 h) than all other tumor types (P <0.001). Consequently, significantly lower red marrow (2.1 +/- 1.0 cGy/mCi versus 4.3 +/- 1.6 cGy/mCi) and whole-body doses (0.5 +/- 0.3 cGy/mCi versus 1.0 +/- 0.4 cGy/mCi) were seen in colorectal cancer patients as compared with other tumor types (P < 0.001). This clearance is probably due to hepatic metabolism of the immune complexes. Clearance rates were especially high in patients with colorectal cancer having large liver metastases and elevated liver enzymes (rapid hepatic clearance with liberation of free I-). In contrast, a disease-stage and plasma CEA-matched cohort of colorectal cancer patients, examined with the 131 I-labeled anti-colon-specific antigen p mAb Mu-9, showed normal murine IgG pharmacokinetics (n=22;3 of them compared intraindividually to MN-14). Only in colorectal cancer patients did complexes between mAb and CEA tend to clear rapidly, whereas Mu-9 had normal kinetics in these patients. This suggests that different CEA-expressing cancer types may produce heterogeneous CEA molecules and that the variability in mAb clearance is due to varying clearance rates of these different circulating CEA subspecies. Disease-related alterations in antibody metabolism are unlikely, given that only anti-CEA antibodies exhibit this phenomenon.

摘要

本研究的目的是探讨在使用抗癌胚抗原(CEA)单克隆抗体(mAb)进行放射免疫检测和放射免疫治疗时,可能影响药代动力学、诊断准确性和剂量测定的因素。对275例表达CEA的肿瘤患者的数据进行了回顾性分析。其中,69例无人类抗鼠抗体的患者(即31例结直肠癌、9例肺癌、7例乳腺癌、4例卵巢癌、6例胰腺癌、9例甲状腺髓样癌、1例胆囊癌、1例唾液腺癌以及1例原发肿瘤来源不明的患者)接受了低蛋白剂量的诊断性研究(0.3 - 2.6 mg蛋白质;6.8 - 28.8 mCi 131I标记的IgG或片段),并在4周内进行了高蛋白剂量的治疗性注射(4.0 - 27.5 mg蛋白质;29.8 - 238.9 mCi)。使用了抗CEA抗体NP - 4(Ka = 10(8)M-1)和MN - 14(ka = 10(9)M-1)。测定了血浆清除率、血浆中放射性的分子组成以及器官和肿瘤中的累积活性。辐射剂量源自医学内照射剂量方案。在低蛋白剂量且血浆CEA处于相似范围时,与循环CEA结合的MN - 14的百分比显著高于NP - 4,这与其更高的亲和力一致。随着蛋白剂量增加,结合作用减弱。然而,靶向敏感性未受影响。发现不同类型癌症患者抗体的清除情况存在显著差异。结直肠癌患者血液(T1/2 = 17.6 +/- 12.6对44.2 +/- 23.7小时)和全身(t½ = 53.2 +/- 30.1对114.6 +/- 59.7小时)中抗体的清除速度明显快于所有其他肿瘤类型(P < 0.001)。因此,与其他肿瘤类型相比,结直肠癌患者的红骨髓剂量(2.1 +/- 1.0 cGy/mCi对4.3 +/- 1.6 cGy/mCi)和全身剂量(0.5 +/- 0.3 cGy/mCi对1.0 +/- 0.4 cGy/mCi)显著更低(P < 0.001)。这种清除可能是由于免疫复合物的肝脏代谢。在有大的肝转移且肝酶升高的结直肠癌患者中清除率尤其高(随着游离I - 的释放快速肝脏清除)。相比之下,一组疾病分期和血浆CEA匹配的结直肠癌患者,用131I标记的抗结肠特异性抗原p mAb Mu - 9进行检测,显示出正常的鼠IgG药代动力学(n = 22;其中3例与MN - 14进行个体内比较)。仅在结直肠癌患者中,mAb与CEA之间的复合物倾向于快速清除,而Mu - 9在这些患者中具有正常的动力学。这表明不同表达CEA的癌症类型可能产生异质性的CEA分子以及mAb清除的变异性是由于这些不同循环CEA亚类的清除率不同。鉴于只有抗CEA抗体表现出这种现象,与疾病相关的抗体代谢改变不太可能。

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