Assessment of the effect of age on macular layer thickness in a healthy Chinese cohort using spectral-domain optical coherence tomography

Detailed assessment of the macular area is critical in the diagnosis and management of a variety of ocular diseases. Traditional investigations such as fundus photography and fluorescein angiography can only provide qualitative and prospective information, therefore being subjective and relatively insensitive to small changes of the macula and unable to provide any cross-sectional or thickness-related data. The introduction of optical coherence tomography (OCT) has made it possible to noninvasively quantify macular structures in vivo with high resolution [1, 2]. In addition, because OCT is easy to use, ensures patient comfort, and is economical, it has become an important diagnostic tool for fundus diseases.

Spectral domain-OCT (SD-OCT) is an advanced modification of time-domain OCT that provides better reproducibility for image acquisition, high-resolution three-dimensional images, and volumetric analyses [3, 4]. Techniques such as enhanced-depth imaging (EDI) permit improved analysis of the living choroid [5]. In addition, advances in layer segmentation algorithms have facilitated the automatic measurement of the thickness of individual retinal layers [6, 7].

Thickness measurement of the macula using SD-OCT has been shown to play an important role in understanding of the anatomy of individual macular layers, each of which has its own normal three-dimensional shape and may be affected in various ways by different diseases. Several studies have investigated morphological abnormalities of the macula in some ocular diseases by using SD-OCT. Macular thickening due to fluid accumulation is found in diabetic retinopathy and central serous chorioretinopathy (CSCR) [8‐10]. The visual acuity of center-involved diabetic macular edema or CSCR eyes may be dependent on the disorganization of the retinal inner layers or the outer nuclear layer (ONL) in the fovea [8, 9]. Macular morphology is also an important parameter for monitoring and staging of glaucoma or age-related macular degeneration (AMD) [11, 12]. Moreover, clinically detected morphologic changes of different retinal layers were identified in many systemic diseases such as multiple sclerosis, [13] Parkinson’s disease, [14] Alzheimer’s disease, [15] and diabetes mellitus with preclinical retinopathy [16]. Therefore, measuring macular thickness by OCT is a powerful tool for physicians to evaluate progression of certain diseases, especially those that involve certain layers.

Recently, SD-OCT was used to study normal retinal and choroid thickness among subjects of different ethnicities, gender, and ages [17‐20]. Age-related reduction in macular thickness was shown in a Caucasian and a Japanese population [18, 21]. However, the aforementioned reports were insufficient to facilitate the detailed analysis of the structure of specific retinal and choroidal layers. Moreover, to our best knowledge, there is no normative database available for the thickness of individual macular layers in the Chinese population.

Therefore, in this study, we used SD-OCT to measure the total retinal thickness (RT), the thickness of individual retinal layers of the macula that were divided into nine sectors, and the subfoveal choroidal thickness (SFCT) including vascular sublayers in 525 ophthalmologically healthy eyes in order to evaluate the effect of age on normal mean regional retinal and subfoveal choroidal layers on the macula.

The study included 525 ophthalmologic healthy eyes of 525 subjects ranging in age from 20 to 87 years (mean age, 44.82 ± 17.74 years). Demographic and ocular features of the study population are presented in Table 1.

The mean thickness of RT and eight individual retinal layers in 9 macular EDTRS sectors of all participants are presented in Appendix: Table 6. IRT was excluded owing to similar results as that of RT (data not shown). After adjusting for spherical equivalence and IOP, no significant correlation was found on foveal RT (P = 0.54) (Table 2). In the fovea, the ONL and RPE correlated negatively with age (Correlation = − 0.15, P < 0.01; Correlation = − 0.09, P = 0.03, respectively) (Table 2); however, the RNFL, INL, and OPL correlated positively with age (Correlation = 0.13, 0.30, 0.10, respectively; all P < 0.05) (Table 2). Regression analysis indicated an increase for the RNFL boundary as well as the INL boundary and a loss for the RPE boundary with increasing age (Beta = 0.13, 0.10, − 0.14, respectively; all P < 0.05) (Table 2).

As shown in Table 3, the total SFCT, thickness of the large choroidal vessel layer (Haller’ s layer), choriocapillaris layer and Sattler’ s layer (medium choroidal vessel layer) in the fovea showed significant negative correlation with age (Correlation = − 0.55, − 0.42, − 0.46, respectively; all P < 0.05). In addition, our study found that SFCT and the thickness of choroidal vascular sublayers decreased linearly with age (Beta = − 0.61, − 0.47, − 0.52, respectively) (all P < 0.05).

Significant age-related reductions were seen for the RT, GCL, and IPL in the pericentral and peripheral rings (all P < 0.05; Tables 4 and 5). Moreover, the OPL of the temporal sector, ONL except the temporal sector in the pericentral ring (both P < 0.05; Table 4), RNFL of both superior and inferior sectors, INL except the superior sector, ONL of all sectors, and PRL + RPE of the inferior sector in the peripheral ring (all P < 0.05; Table 5) showed significant decreases with respect to age. However, significant age-related increase was demonstrated in the RNFL of the temporal sector, INL and OPL of the nasal sector, RPE of all sectors in the pericentral ring (all P < 0.05; Table 4), RNFL of the temporal sector, OPL of the nasal sector, and RPE of the superior and temporal sectors in the peripheral ring (all P < 0.05; Table 5).

In this study, consistent with previous reports, [23‐25] no significant correlation was found between age and foveal RT. However, the ONL, RPE and choroid vascular sublayers in this region showed significant age-related thinning, accompanied with age-related thickness of RNFL, INL, and OPL. To our best knowledge, we believe this is the first study to report the detailed age-related changes of foveal microstructure. On comparing with total thickness, assessment of macular layers provides a higher diagnostic power. The most significant observation herein was the age-related thinning of foveal ONL, RPE and choroid measurements even in ophthalmologically healthy subjects, which could be a potential anatomic predisposing factor for monitoring the age-related diseases in this eye region. The atrophy of RPE and choroid layer in the central retina is a feature of early/intermediate AMD, the incidence of which is increased with age. A 32% loss in the RPE/PRL thickness and a 22% loss in ONL thickness were found over the drusen as compared to the adjacent drusen-free regions in AMD patients [26]. The choriocapillaris degenerates in early stages of AMD, before loss of photoreceptor cells or RPE [12]. Although AMD is a complicated process that involves both age-related change and tissue damage caused by multiple stresses, age plays the most important role [27]. Functionally normal RPE and choroidal vasculature play a critical role in maintaining retinal health. Thinner RPE and choroid layer thickness may be anatomic features lead to increased risk in AMD. Our results showed that assessment of the foveal layer thickness with OCT in ophthalmologically healthy aged subjects’ eyes may lead to early identification and treatment of AMD. Moreover, further investigations are needed on the mechanism of age-related variations of the ONL, RPE, RNFL, INL, and OPL in the fovea.

We have observed significant age-associated reductions of RT in the pericentral and peripheral rings that were distinct from the foveal results; these results were consistent with previous studies [19, 28, 29]. Notably, age-related changes of GCL, IPL, and ONL in the region likely contribute to this result. Parikh et al. [30] reported that age was related to the loss of neurons or glial cells in the inner retina, which may be responsible for the SD-OCT–examination outcome in this area.

Several studies have shown that assessment of GCL thickness could be a surrogate method to evaluate glaucomatous damage [31]. In this study, the observed age-related variation in GCL thickness in this ophthalmologically healthy cohort is a reminder that GCL thinning requires more accurate quantification before widespread adoption as a surrogate for glaucoma assessment.

The thickness of RPE in the pericentral and peripheral regions was significantly increased with aging. Many pathological changes led to the thickening of the RPE, which included the density of residual bodies and accumulation of lipofuscin, accumulation of basal deposits on or within the Bruch’s membrane, formation of drusen, and thickening of the Bruch’s membrane [32]. The age-related variation of RPE in the macular region requires future investigation.

This study has some limitations. The small sample size might have introduced some bias. Our data are limited to Chinese ethnicity and need to be tested in other ethnic groups in the future.

Using SD-OCT, we assessed age-related thinning of ONL, RPE, and choroidal layers accompanied with thickened RNFL, INL, and OPL of the fovea in an ophthalmologically healthy Chinese cohort. The variations of individual layers in the fovea may be related to age-independent RT. It is speculated that the age-related reductions of RT in the pericentral and peripheral rings were associated with age-related thinning of GCL, IPL and ONL in these regions. Regular monitoring of the macular architecture using SD-OCT in ophthalmologically healthy people, especially among the aged population, should be considered in future evaluations.