Freda P U, Post K D, Powell J S, Wardlaw S L
Department of Medicine, Columbia College of Physicians and Surgeons, New York, New York 10032, USA.
J Clin Endocrinol Metab. 1998 Nov;83(11):3808-16. doi: 10.1210/jcem.83.11.5266.
Traditionally, suppression of GH measured by polyclonal RIA to less than 2.0 microg/L after oral glucose was accepted as evidence of remission after transsphenoidal surgery for acromegaly. Recently, with newer, more sensitive GH assays, a cut-off of less than 1.0 microg/L has been suggested. With the development of accurate insulin-like growth factor I (IGF-I) and IGF-binding protein-3 (IGFBP-3) assays, additional tools are now available for assessing postoperative GH secretion. There has, however, never been a systematic comparison of sensitive GH, IGF-I, and IGFBP-3 assays in defining disease status in a large cohort of postoperative patients with acromegaly. Therefore, we evaluated how the use of modern assays impacts on our assessment of disease activity in these patients. Sixty postoperative subjects with acromegaly and 25 age-matched healthy subjects were evaluated with nadir GH levels after 100 g oral glucose as well as baseline IGF-I and IGFBP-3 levels. GH was assayed by polyclonal RIA, sensitive immunoradiometric assay (IRMA), and highly sensitive enzyme-linked immunosorbent assay. The mean nadir GH determined by IRMA was 0.09 +/- 0.004 microg/L in the healthy subjects, with the upper limit of the normal nadir being 0.14 microg/L (mean + 2 SD). Subjects with acromegaly were divided into those with active disease (n = 22), defined by elevated IGF-I levels, and those in remission (n = 38), defined by normal IGF-I levels. GH determined by IRMA failed to suppress into the normal range defined by our healthy subjects in all patients with active disease; nadir GH determined by IRMA ranged from 0.33-5.0 microg/L in this group. In 50% of the active group, nadir GH levels determined by IRMA were less than 1.0 microg/L, a GH nadir previously considered normal by strict criteria. When nadir GH levels in the subjects with active disease were measured by polyclonal RIA, there was overlap with the range of RIA values in the healthy subjects. Thus, the IRMA was superior to the RIA in that the overlap between these two groups was eliminated. Subjects with acromegaly in remission included those with normal GH suppression (n = 23; mean nadir GH by IRMA, 0.10 +/- 0.006 microg/L) and others with abnormal GH suppression by IRMA (n = 15; mean nadir GH by IRMA, 0.35 +/- 0.07 microg/L). The latter group may have persistent GH dysregulation detected by the sensitive IRMA. GH levels measured by enzyme-linked immunosorbent assay confirmed the IRMA results. IGFBP-3 levels were significantly higher in subjects with active acromegaly (4940 +/- 301 microg/L) vs. those in healthy subjects (2887 +/- 153 microg/L; P < 0.0001) and those in the subjects in remission (2966 microg/L; P < 0.0001). IGFBP-3 levels correlated overall with IGF-I levels (r = 0.765; P < 0.0001), but IGFBP-3 levels were not predictive of disease status because 32% of the subjects with active acromegaly had normal IGFBP-3 levels. In addition, failure of GH to suppress adequately was not associated with a higher IGFBP-3 level among the subjects in remission. These data indicate that the IRMA is superior to the RIA in distinguishing between patients with active disease (defined by elevated IGF-I levels) and healthy subjects. We also show that GH levels after oral glucose measured with highly sensitive GH assays can be much lower in subjects with active disease than previously believed; values less than 1.0 microg/L may be found in up to 50% of patients. In addition, in 39% of patients in apparent remission with normal IGF-I levels, GH determined by highly sensitive assays fails to suppress normally; it remains to be determined whether these patients are at higher risk for recurrence of active disease.
传统上,经蝶窦手术治疗肢端肥大症后,口服葡萄糖后用多克隆放射免疫分析法(RIA)测得的生长激素(GH)抑制至低于2.0μg/L被视为缓解的证据。近来,随着更新的、更敏感的GH检测方法的出现,有人提出将临界值设定为低于1.0μg/L。随着准确的胰岛素样生长因子I(IGF-I)和IGF结合蛋白-3(IGFBP-3)检测方法的发展,现在有了更多用于评估术后GH分泌的工具。然而,在一大群肢端肥大症术后患者中,从未对敏感的GH、IGF-I和IGFBP-3检测方法在定义疾病状态方面进行过系统比较。因此,我们评估了使用现代检测方法如何影响我们对这些患者疾病活动的评估。对60例肢端肥大症术后患者和25例年龄匹配的健康受试者进行了评估,测定口服100g葡萄糖后的最低GH水平以及基线IGF-I和IGFBP-3水平。GH采用多克隆RIA、敏感免疫放射分析法(IRMA)和高灵敏度酶联免疫吸附测定法进行检测。健康受试者经IRMA测定的平均最低GH为0.09±0.004μg/L,正常最低值的上限为0.14μg/L(平均值+2标准差)。肢端肥大症患者分为疾病活动组(n = 22),由IGF-I水平升高定义,以及缓解组(n = 38),由IGF-I水平正常定义。在所有疾病活动的患者中,经IRMA测定的GH未能抑制到我们健康受试者定义的正常范围内;该组经IRMA测定的最低GH范围为0.33 - 5.0μg/L。在活动组的50%患者中,经IRMA测定的最低GH水平低于1.0μg/L,这一GH最低值以前按严格标准被认为是正常的。当用多克隆RIA测量疾病活动患者的最低GH水平时,与健康受试者的RIA值范围有重叠。因此,IRMA优于RIA,因为消除了这两组之间的重叠。肢端肥大症缓解患者包括GH抑制正常的患者(n = 23;经IRMA测定的平均最低GH为0.10±0.006μg/L)和其他经IRMA测定GH抑制异常的患者(n = 15;经IRMA测定的平均最低GH为0.35±0.07μg/L)。后一组可能通过敏感的IRMA检测到持续的GH调节异常。用酶联免疫吸附测定法测量的GH水平证实了IRMA的结果。活动期肢端肥大症患者的IGFBP-3水平(4940±301μg/L)显著高于健康受试者(2887±153μg/L;P < 0.0001)和缓解期患者(2966μg/L;P < 0.0001)。IGFBP-总体上与IGF-I水平相关(r = 0.765;P < 0.0001),但IGFBP-3水平不能预测疾病状态,因为32%的疾病活动期肢端肥大症患者IGFBP-3水平正常。此外,在缓解期患者中,GH未能充分抑制与较高的IGFBP-3水平无关。这些数据表明,在区分疾病活动患者(由IGF-I水平升高定义)和健康受试者方面,IRMA优于RIA。我们还表明,用高灵敏度GH检测方法测得的口服葡萄糖后GH水平在疾病活动患者中可能比以前认为的要低得多;高达50%的患者可能出现低于1.0μg/L的值。此外,在39%的IGF-I水平正常、明显缓解的患者中,经高灵敏度检测方法测定的GH未能正常抑制;这些患者是否有更高的疾病活动复发风险仍有待确定。
