University Paris-Est Creteil, Hôpital Henri Mondor, 94010 Creteil, France.
J Bone Joint Surg Am. 2012 Jan 18;94(2):156-62. doi: 10.2106/JBJS.J.00919.
Osteonecrosis of the humeral head is a frequent complication in adults with sickle cell disease. However, little is known about the rate of, and the factors influencing, progression of symptomatic shoulder osteonecrosis in patients with this disease.
Eighty-two adult patients with sickle cell disease and symptomatic osteonecrosis of the humeral head (104 shoulders) were identified with magnetic resonance imaging (MRI) between 1985 and 1993. Nineteen of the eighty-two patients were homozygous for hemoglobin S (S/S genotype), thirty-seven had hemoglobin S/hemoglobin C (S/C), and twenty-six had hemoglobin S/beta-thalassemia (S/T). Shoulder osteonecrosis was graded with the method of Cruess with an adaptation for MRI as proposed by Steinberg et al. for hip osteonecrosis. Annual radiographs were obtained. At the initial evaluation, thirty-eight symptomatic shoulders were designated as stage I (with osteonecrosis seen only on MRI), forty-two symptomatic shoulders were designated as stage II (radiographic evidence without collapse), and twenty-four symptomatic shoulders were designated as stage III or IV (a crescent line or collapse).
Partial or total repair with a decrease in the size of the osteonecrotic lesion or in the stage was never observed on MRI. At the time of the most recent follow-up (average, twenty years; range, fifteen to twenty-four years), collapse had occurred in eighty-nine shoulders (86%). The mean interval between the onset of pain and collapse was six years (range, six months to seventeen years; median, eight years). Of the 104 symptomatic shoulders, sixty-three (61%) with collapse worsened clinically until surgical treatment was needed. The principal risk factors for development of shoulder osteonecrosis in adults with sickle cell disease were the presence of hip osteonecrosis and the S/T or S/C genotype. The rate and risk of progression of the lesion until collapse occurred were significantly related to the S/S genotype, to a stage of II, to a large size of the osteonecrotic lesion, and to a medial or posterior location of the lesion.
Untreated symptomatic shoulder osteonecrosis related to sickle cell disease has a high likelihood of progressing to humeral head collapse, and the natural evolution in the long term requires surgical treatment for many of these patients.
肱骨头骨坏死是镰状细胞病成人的常见并发症。然而,对于患有这种疾病的患者,症状性肩骨坏死的进展率以及影响进展的因素知之甚少。
1985 年至 1993 年期间,通过磁共振成像(MRI)确定了 82 例镰状细胞病伴症状性肱骨头骨坏死(104 肩)的成年患者。82 例患者中,19 例为血红蛋白 S 纯合子(SS 基因型),37 例为血红蛋白 S/血红蛋白 C(SC),26 例为血红蛋白 S/β-地中海贫血(ST)。采用 Cruess 分级方法对肩骨坏死进行分级,并采用 Steinberg 等人为髋关节骨坏死提出的 MRI 适应性方法进行改良。每年拍摄 X 线片。在初次评估时,将 38 个有症状的肩膀指定为 I 期(仅在 MRI 上可见骨坏死),42 个有症状的肩膀指定为 II 期(有影像学证据但无塌陷),24 个有症状的肩膀指定为 III 期或 IV 期(新月形线或塌陷)。
MRI 从未观察到部分或完全修复,伴有骨坏死病变的大小减小或分期降低。在最近的随访时(平均 20 年;范围 15-24 年),89 个肩膀(86%)发生了塌陷。疼痛发作与塌陷之间的平均间隔为 6 年(范围 6 个月至 17 年;中位数为 8 年)。在 104 个有症状的肩膀中,有 63 个(61%)塌陷肩膀的临床症状恶化,需要手术治疗。镰状细胞病成人发生肩骨坏死的主要危险因素是髋骨坏死以及 ST 或 SC 基因型。病变进展直至塌陷的发生率和风险与 SS 基因型、II 期、骨坏死病变大、病变位于内侧或后侧显著相关。
未治疗的镰状细胞病相关症状性肩骨坏死很可能进展为肱骨头塌陷,长期自然演变需要对许多此类患者进行手术治疗。
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