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儿童外周血淋巴细胞生长激素受体的表达:生长受损临床状况下的评估

Expression of growth hormone receptor by peripheral blood lymphocytes in children: evaluation in clinical conditions of impaired growth.

作者信息

Valerio G, Bond H M, Badolato R, Petrella A, Di Maio S, Salerno M, Waters M J, Venuta S, Tenore A

机构信息

Department of Pediatrics (DPMSC), University of Udine, School of Medicine, Italy.

出版信息

Clin Endocrinol (Oxf). 1997 Sep;47(3):329-35. doi: 10.1046/j.1365-2265.1997.2571066.x.

Abstract

OBJECTIVE

It is widely accepted that the haematopoietic system is a target of growth hormone action and that GH may act as a lymphokine. The expression of GH receptors (GHR) on human peripheral blood lymphocytes (PBL) has been reported previously in adult donors by dual fluorochrome flow cytometry. The aim of this study was to apply the cytofluorimetric method to the analysis of GHR expression on PBL in various human conditions characterized by different patterns of growth due to age or physiopathological conditions.

SUBJECTS AND DESIGN

PBL from 38 normal (control) subjects (7 newborns, 18 prepubertal children, 13 adults) were studied in order to provide age-related physiological data. Twenty-two short children (18 with idiopathic short stature, 4 with Ullrich-Turner syndrome) were studied to determine the expression of GHR in conditions of impaired longitudinal growth which may or may not require GH treatment.

METHODS

Analysis was performed using a fluorescein isothiocyanate (FITC)-conjugated antibody specific for the GHR (mAb263) and phycoerythrin (PE)-anti CD2 (T and natural killer cells) or PE-anti CD2 (B cells) in dual fluorochrome flow cytometric assays. Results were expressed as mean fluorescent intensity (MFI).

RESULTS

Adult CD2+ coils exhibited a significantly higher GHR expression (MFI 347 +/- 40) than that expressed in children and newborns (MFI 285 +/- 36 and 299 +/- 41, respectively, P < 0.001). A significantly increased expression of GHR on CD2+ cells was also found in short children (MFI 330 +/- 42 vs 285 42- 36, respectively; P < 0.002), whereas Ullrich-Turner syndrome patients did not show any difference from their age and gender matched controls (254 +/- 52 and 288 +/- 40, respectively). A negative relationship was found between GHR expression on CD2+ cells and height-SDS (r - 0.54, P < 0.0001) or BMI (r - 0.4, P < 0.015) in controls and short children, independent of their GH secretory status. Expression of GHR and CD20+ cells was higher than that expressed on CD2+ cells in all subjects. No appreciable differences were found in the MFI levels of GHR expression on CD20+ cells either among the different age group controls or between short children or Ullrich-Turner syndrome patients. A significant downregulation of expression was shown in CD20+ (P < 0.008) but not CD2+ cells after 6 months of GH treatment in 6 short children who had a poor response to GH provocative tests.

CONCLUSIONS

GH receptor expression on immune cells in non-syndromic short children appears to be inversely related to the linear growth expression and BMI of the subjects, contrary to findings with hepatic derived serum GHBP. This finding may reflect alternate exon usage in lymphoid cells, and indicates that GH has a distinctive role in the immune system.

摘要

目的

造血系统是生长激素作用的靶器官,且生长激素可能作为一种淋巴因子,这一观点已被广泛接受。此前通过双荧光流式细胞术已报道了成年供者外周血淋巴细胞(PBL)上生长激素受体(GHR)的表达情况。本研究的目的是应用细胞荧光分析方法,分析在因年龄或生理病理状况导致生长模式不同的各种人体条件下,PBL上GHR的表达情况。

对象与设计

研究了38名正常(对照)受试者(7名新生儿、18名青春期前儿童、13名成年人)的PBL,以提供与年龄相关的生理数据。研究了22名身材矮小儿童(18名特发性矮小,4名 Ullrich-Turner 综合征),以确定在纵向生长受损且可能需要或不需要生长激素治疗的情况下GHR的表达情况。

方法

在双荧光流式细胞分析中,使用针对GHR的异硫氰酸荧光素(FITC)偶联抗体(单克隆抗体263)和藻红蛋白(PE)-抗CD2(T细胞和自然杀伤细胞)或PE-抗CD20(B细胞)进行分析。结果以平均荧光强度(MFI)表示。

结果

成年CD2⁺细胞表现出比儿童和新生儿显著更高的GHR表达(MFI分别为347±40、285±36和299±41,P<0.001)。身材矮小儿童的CD2⁺细胞上GHR表达也显著增加(MFI分别为330±42和285±36;P<0.002),而Ullrich-Turner综合征患者与年龄和性别匹配的对照组相比无差异(分别为254±52和288±40)。在对照组和身材矮小儿童中,CD2⁺细胞上的GHR表达与身高标准差评分(r=-0.54,P<0.0001)或体重指数(r=-0.4,P<0.015)呈负相关,与他们的生长激素分泌状态无关。所有受试者中,GHR在CD20⁺细胞上的表达高于在CD2⁺细胞上的表达。在不同年龄组的对照组之间,以及身材矮小儿童或Ullrich-Turner综合征患者之间,CD20⁺细胞上GHR表达的MFI水平未发现明显差异。6名对生长激素激发试验反应不佳的身材矮小儿童接受生长激素治疗6个月后,CD20⁺细胞(P<0.008)而非CD2⁺细胞的表达出现显著下调。

结论

非综合征性身材矮小儿童免疫细胞上的生长激素受体表达似乎与受试者 的线性生长和体重指数呈负相关,这与肝脏来源的血清生长激素结合蛋白的研究结果相反。这一发现可能反映了淋巴细胞中可变外显子的使用情况,并表明生长激素在免疫系统中具有独特作用。

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