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细胞模式和眼眶脂肪受累可能是单纯特发性眼眶炎症综合征患者皮质类固醇治疗失败的危险因素:来自法国前瞻性队列研究的经验教训(第二部分)。

Cellular pattern and orbital fat involvement are possible risk factors for the failure of corticosteroids in patients with pure idiopathic orbital inflammation syndrome: lessons from the French prospective cohort study (part II).

机构信息

Médecine Interne, Hôpital Avicenne, Assistance Publique-Hôpitaux de Paris (APHP), Bobigny, France.

Médecine Interne, Centre National de Référence des Syndromes Hyperéosinophiliques (CEREO), Hôpital Foch, Suresnes, France.

出版信息

BMJ Open Ophthalmol. 2024 Sep 23;9(1):e001663. doi: 10.1136/bmjophth-2024-001663.

Abstract

PURPOSE

To better characterise the effects of corticosteroids on the course of pure idiopathic orbital inflammation syndrome (pIOIS).

METHODS

This was a national, multicentre, prospective, non-interventional cohort study (). Among the 35 patients with histologically proven orbital inflammation who had previously been studied for their IgG4 immunostaining status, we selected those with a negative IgG4 status (ie, pIOIS) who received corticosteroids as single first-line treatment. Clinical, morphological and pathological findings at diagnosis and during follow-up from treatment initiation to study completion were analysed. Patients were assessed for their response to prednisone after the 24-month prospective phase in terms of remission (≤10 mg/d) or failure (>10 mg/d). Daily standard doses of prednisone (DSDP) were calculated at different time-points and compared between response groups.

RESULTS

Of the 17 patients with pIOIS included in the final analysis, two-thirds received corticosteroids only. DSDP (mg/kg-day) were significantly higher at the time of failure in eight patients (47%) than in nine (53%) remitting at M24 (0.16 vs 0.045; p: 0.03). Notably, patients with pIOIS with a cellular pattern or orbital fat involvement tended to receive higher daily corticosteroid doses in the event of failure than remission (0.16 vs 0.045 and 0.12 vs 0.042, respectively). During treatment, maximal DSDP was 0.52 in failed patients.

CONCLUSION

The highest corticosteroid doses were insufficient to prevent failure in patients with pIOIS, particularly in those with a cellular pattern or orbital fat involvement. Large-scale interventional studies are now necessary to clarify prognostic factors and optimise corticosteroid management in patients with pIOIS.

摘要

目的

更好地描述皮质类固醇对单纯特发性眼眶炎症综合征(pIOIS)病程的影响。

方法

这是一项全国性、多中心、前瞻性、非干预性队列研究()。在 35 名经组织学证实患有眼眶炎症且 IgG4 免疫染色状态先前已被研究过的患者中,我们选择了 IgG4 状态阴性(即 pIOIS)的患者,他们接受皮质类固醇作为单一一线治疗。分析了诊断时以及从治疗开始到研究完成时的临床、形态和病理发现。在 24 个月的前瞻性阶段后,根据缓解(≤10mg/d)或失败(>10mg/d)评估患者对泼尼松的反应。在不同时间点计算每日标准泼尼松剂量(DSDP),并比较反应组之间的差异。

结果

在最终分析的 17 名 pIOIS 患者中,三分之二仅接受皮质类固醇治疗。在 8 名(47%)失败患者中,DSDP(mg/kg-day)在 M24 时明显高于 9 名(53%)缓解患者(0.16 对 0.045;p:0.03)。值得注意的是,在失败和缓解患者中,具有细胞模式或眶脂肪受累的 pIOIS 患者接受更高的每日皮质类固醇剂量的趋势(0.16 对 0.045 和 0.12 对 0.042)。在治疗期间,失败患者的最大 DSDP 为 0.52。

结论

在 pIOIS 患者中,最高的皮质类固醇剂量不足以预防失败,特别是在具有细胞模式或眶脂肪受累的患者中。现在需要进行大规模的干预性研究,以明确预后因素并优化 pIOIS 患者的皮质类固醇管理。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/745f/11418487/9796b5131c4b/bmjophth-9-1-g001.jpg

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