Flaxel C J, Jay M, Thiselton D L, Nayudu M, Hardcastle A J, Wright A, Bird A C
Currently affiliated with the University of Southern California, Doheny Eye Institute, Los Angeles, CA, USA.
Br J Ophthalmol. 1999 Oct;83(10):1144-8. doi: 10.1136/bjo.83.10.1144.
X linked retinitis pigmentosa (XLRP) has two genetic loci known as "RP2" and "RP3". Clinical features reported to differentiate RP2 from RP3 include a higher prevalence of myopia and primary cone dysfunction in RP2, and late onset night blindness and tapetal reflex in RP3. Members from 14 XLRP families were examined in an attempt to verify these differences.
16 affected males and 37 females from 14 XLRP families assigned as either RP2 or RP3 by haplotype analysis and/or by heterogeneity analysis were examined. Members of all 14 families who were willing to participate but unavailable for examination were contacted and detailed interviews carried out.
No clear phenotypic differences were found that could be used to reliably differentiate RP2 from RP3 with respect to myopia and onset of night blindness. The tapetal reflex was also found to be present in carriers of both RP2 and RP3.
XLRP is a heterogeneous class of rod degenerative disorders with no clear phenotypic differentiation between the two genetic loci RP2 and RP3. There is a continuum of clinical presentations which can be seen in both RP2 and RP3, but the features within a given family tend to be consistent. However, interfamilial variability is prevalent leading to a wide range of clinical presentations and more than one abnormal allele at each gene locus cannot be excluded.
X连锁视网膜色素变性(XLRP)有两个已知的基因位点,即“RP2”和“RP3”。据报道,区分RP2和RP3的临床特征包括RP2中近视和原发性视锥功能障碍的患病率较高,以及RP3中迟发性夜盲和脉络膜反光。对14个XLRP家系的成员进行了检查,以试图验证这些差异。
对14个XLRP家系中通过单倍型分析和/或异质性分析被指定为RP2或RP3的16名患病男性和37名女性进行了检查。与所有14个愿意参与但无法接受检查的家系成员进行了联系,并进行了详细访谈。
未发现可用于可靠区分RP2和RP3在近视和夜盲发病方面的明显表型差异。还发现RP2和RP3的携带者均存在脉络膜反光。
XLRP是一类异质性的视杆细胞退行性疾病,在两个基因位点RP2和RP3之间没有明显的表型分化。在RP2和RP3中均可观察到一系列连续的临床表现,但在给定家系中的特征往往是一致的。然而,家系间变异性普遍存在,导致临床表现范围广泛,且不能排除每个基因位点存在多个异常等位基因的情况。