Tai Tak Yee Tania, Damani Mausam R, Vo Rosalind, Rayner Sylvia A, Glasgow Ben J, Hofbauer John D, Casey Richard, Aldave Anthony J
The Jules Stein Eye Institute, David Geffen School of Medicine, The University of California at Los Angeles, Los Angeles, CA 90095, USA.
Cornea. 2009 Jun;28(5):589-93. doi: 10.1097/ICO.0b013e31818c9003.
To report the identification and characterization of stromal amyloid deposits in patients with keratoconus.
The excised corneal buttons from 2 patients diagnosed clinically with keratoconus underwent histochemical analysis with Masson trichrome, Congo red, Alcian blue, and periodic acid-Schiff stains, and immunohistochemical analysis for the transforming growth factor beta-induced gene (TGFBI) protein product (TGFBIp), prealbumin, lysozyme, and kappa and lambda light chain expression. After the collection of DNA from both patients, exons 4, 11, 12, 13 and 14 of TGFBI were amplified and sequenced to search for mutations previously associated with dystrophic corneal stromal amyloid deposition.
Light microscopic examination of the corneal buttons revealed stromal thinning, epithelial basement membrane abnormalities, and focal disruption of Bowman layer. Multiple stromal deposits were identified that stained red with Masson trichrome, pink with periodic acid-Schiff, and red with Congo red; the Congo red-stained deposits demonstrated birefringence and dichroism with crossed polarizing lenses. Immunohistochemical staining demonstrated reactivity of the stromal deposits with antibodies to TGFBIp but no reactivity with antibodies against prealbumin, lysozyme, or kappa and lambda light chains. Screening of TGFBI exons 4, 11, 12, 13, and 14 revealed 2 previously identified single nucleotide polymorphisms present in the heterozygous state in both individuals but no other coding region variants.
Two cases of keratoconus with clinically unsuspected, presumed secondary stromal amyloid deposition are described. Although TGFBIp is identified in the stromal deposits, no previously reported amyloidogenic mutations are identified in TGFBI in either affected individual, indicating a previously undescribed mechanism of stromal amyloid deposition.
报告圆锥角膜患者基质淀粉样沉积物的鉴定与特征。
对2例临床诊断为圆锥角膜患者切除的角膜纽扣组织进行Masson三色染色、刚果红染色、阿尔辛蓝染色和过碘酸-希夫染色的组织化学分析,以及对转化生长因子β诱导基因(TGFBI)蛋白产物(TGFBIp)、前白蛋白、溶菌酶以及κ和λ轻链表达进行免疫组织化学分析。从两名患者采集DNA后,对TGFBI的第4、11、12、13和14外显子进行扩增和测序,以寻找先前与营养不良性角膜基质淀粉样沉积相关的突变。
角膜纽扣组织的光学显微镜检查显示基质变薄、上皮基底膜异常以及Bowman层局灶性破坏。鉴定出多个基质沉积物,Masson三色染色呈红色、过碘酸-希夫染色呈粉红色、刚果红染色呈红色;刚果红染色的沉积物在交叉偏振镜下显示双折射和二色性。免疫组织化学染色显示基质沉积物与抗TGFBIp抗体有反应,但与抗前白蛋白、溶菌酶或κ和λ轻链抗体无反应。对TGFBI第4、11、12、13和14外显子的筛查显示,两名个体均存在杂合状态的2个先前已鉴定的单核苷酸多态性,但未发现其他编码区变异。
描述了2例临床未怀疑的、推测为继发性基质淀粉样沉积的圆锥角膜病例。尽管在基质沉积物中鉴定出TGFBIp,但在任何一名受累个体的TGFBI中均未发现先前报道的淀粉样变性突变,提示存在一种先前未描述的基质淀粉样沉积机制。