Brehm Anja, Liu Yin, Sheikh Afzal, Marrero Bernadette, Omoyinmi Ebun, Zhou Qing, Montealegre Gina, Biancotto Angelique, Reinhardt Adam, Almeida de Jesus Adriana, Pelletier Martin, Tsai Wanxia L, Remmers Elaine F, Kardava Lela, Hill Suvimol, Kim Hanna, Lachmann Helen J, Megarbane Andre, Chae Jae Jin, Brady Jilian, Castillo Rhina D, Brown Diane, Casano Angel Vera, Gao Ling, Chapelle Dawn, Huang Yan, Stone Deborah, Chen Yongqing, Sotzny Franziska, Lee Chyi-Chia Richard, Kastner Daniel L, Torrelo Antonio, Zlotogorski Abraham, Moir Susan, Gadina Massimo, McCoy Phil, Wesley Robert, Rother Kristina I, Hildebrand Peter W, Brogan Paul, Krüger Elke, Aksentijevich Ivona, Goldbach-Mansky Raphaela
J Clin Invest. 2015 Nov 2;125(11):4196-211. doi: 10.1172/JCI81260. Epub 2015 Oct 20.
Autosomal recessive mutations in proteasome subunit β 8 (PSMB8), which encodes the inducible proteasome subunit β5i, cause the immune-dysregulatory disease chronic atypical neutrophilic dermatosis with lipodystrophy and elevated temperature (CANDLE), which is classified as a proteasome-associated autoinflammatory syndrome (PRAAS). Here, we identified 8 mutations in 4 proteasome genes, PSMA3 (encodes α7), PSMB4 (encodes β7), PSMB9 (encodes β1i), and proteasome maturation protein (POMP), that have not been previously associated with disease and 1 mutation in PSMB8 that has not been previously reported. One patient was compound heterozygous for PSMB4 mutations, 6 patients from 4 families were heterozygous for a missense mutation in 1 inducible proteasome subunit and a mutation in a constitutive proteasome subunit, and 1 patient was heterozygous for a POMP mutation, thus establishing a digenic and autosomal dominant inheritance pattern of PRAAS. Function evaluation revealed that these mutations variably affect transcription, protein expression, protein folding, proteasome assembly, and, ultimately, proteasome activity. Moreover, defects in proteasome formation and function were recapitulated by siRNA-mediated knockdown of the respective subunits in primary fibroblasts from healthy individuals. Patient-isolated hematopoietic and nonhematopoietic cells exhibited a strong IFN gene-expression signature, irrespective of genotype. Additionally, chemical proteasome inhibition or progressive depletion of proteasome subunit gene transcription with siRNA induced transcription of type I IFN genes in healthy control cells. Our results provide further insight into CANDLE genetics and link global proteasome dysfunction to increased type I IFN production.
蛋白酶体亚基β8(PSMB8)的常染色体隐性突变可导致免疫失调疾病——伴有脂肪营养不良和体温升高的慢性非典型嗜中性皮肤病(CANDLE),该基因编码诱导型蛋白酶体亚基β5i,CANDLE被归类为蛋白酶体相关自身炎症综合征(PRAAS)。在此,我们在4个蛋白酶体基因(PSMA3,编码α7;PSMB4,编码β7;PSMB9,编码β1i;蛋白酶体成熟蛋白(POMP))中鉴定出8种此前未与疾病相关的突变,以及1种此前未报道的PSMB8突变。1例患者为PSMB4突变的复合杂合子,来自4个家庭的6例患者为1种诱导型蛋白酶体亚基错义突变和1种组成型蛋白酶体亚基突变的杂合子,1例患者为POMP突变的杂合子,从而确立了PRAAS的双基因和常染色体显性遗传模式。功能评估显示,这些突变对转录、蛋白质表达、蛋白质折叠、蛋白酶体组装以及最终的蛋白酶体活性有不同程度的影响。此外,通过小干扰RNA(siRNA)介导敲低健康个体原代成纤维细胞中的相应亚基,可重现蛋白酶体形成和功能的缺陷。无论基因型如何,患者分离的造血和非造血细胞均表现出强烈的IFN基因表达特征。此外,化学性蛋白酶体抑制或用siRNA逐步减少蛋白酶体亚基基因转录可诱导健康对照细胞中I型IFN基因的转录。我们的研究结果为深入了解CANDLE遗传学提供了更多信息,并将整体蛋白酶体功能障碍与I型IFN产生增加联系起来。
