Dysfunction of Natural Killer Activity in a Family with Chronic Fatigue Syndrome

Paul H. Levine , Theresa L. Whiteside , Diana Friberg , John Bryant , Ginga Colclough , Ronald B. Herberman
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引用次数: 73

Abstract

A family was identified with 5 of 6 siblings and 3 other immediate family members who had developed chronic fatigue syndrome (CFS) as adults. All 8 met criteria for the CFS case definition as recommended by the Centers for Disease Control and Prevention. Sixty-eight blood samples were obtained over a period of 2 years from 20 family members (8 affected, 12 unaffected) and 8 normal controls. All blood samples were tested for NK activity in 4-h51Cr-release assays and for the number of circulating CD3–CD56+and CD3–CD16+by flow cytometry. NK activity of the affected immediate family members (cases,n= 8) was significantly lower (P= 0.006, two-sided) than that of the concurrently tested normal controls. The results for unaffected family members were intermediate between these two groups, and the pairwise comparison of unaffected family members to either cases or controls showed no statistically significant difference (P= 0.29, two-sided). No differences were seen between the groups in the absolute number of CD3–CD56+or CD3–CD16+lymphocytes in the peripheral blood. Familial CFS was associated withpersistentlylow NK activity, which was documented in 6/8 cases and in 4/12 unaffected family members. In the family with 5 of 6 siblings who had documented CFS, 2 of their offspring had pediatric malignancies. Low NK activity in this family may be a result of a genetically determined immunologic abnormality predisposing to CFS and cancer.

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慢性疲劳综合征家庭中自然杀手活动的功能障碍
一个家庭的6个兄弟姐妹中有5个和其他3个直系亲属在成年后患有慢性疲劳综合征。所有8例均符合疾病控制和预防中心推荐的CFS病例定义标准。在2年的时间里,从20名家庭成员(8名受影响,12名未受影响)和8名正常对照中获得68份血液样本。用4- h51cr释放法检测NK活性,用流式细胞术检测循环CD3-CD56 +和CD3-CD16 +的数量。直系亲属(病例,n= 8)的NK活性显著低于同期检测的正常对照(P= 0.006,双侧)。未患病家庭成员的结果介于两组之间,未患病家庭成员与病例或对照组的两两比较均无统计学差异(P= 0.29,双侧)。两组外周血中CD3-CD56 +和CD3-CD16 +淋巴细胞的绝对数量没有差异。家族性CFS与持续低NK活性相关,在6/8例和4/12未受影响的家庭成员中有记录。在6个兄弟姐妹中有5个患有慢性疲劳综合症的家庭中,他们的2个后代患有儿科恶性肿瘤。低NK活性在这个家庭可能是一种遗传决定的免疫异常,易患CFS和癌症的结果。
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