FD is an increasingly recognized but still underdiagnosed lysosomal storage disorder. Those who has non-classical variants due to missense and splicing mutations often has milder disease severity and later onset of clinical manifestations due to higher residual alpha-galactosidase activity. 37.8% of our subjects are identified and diagnosed with FD through family cascade screening. Recognition of these later-onset FD patients is crucial as it would permit expeditious cascade screening and timely therapeutic intervention. [14] GLA enzyme assay is the recommended diagnostic test for male patients but it is less sensitive in female, whom would require GLA gene sequencing to make the diagnosis. Both tests, however, are not readily accessible in every institution. In this study, we explore the utility of BA diameter as an easily obtainable MRI biomarker for FD screening and prognosis.
This is the first study on VBD and FD in the Chinese population. We demonstrated that BA diameter was significantly enlarged compared to general population in both stroke and non-stroke subgroups. In a study conducted in Germany with 87 FD patients, investigators demonstrated a BA diameter > 3.2mm could distinguish FD from normal controls with a high sensitivity of 87% and specificity of 86%, but it failed to find a difference in BA diameter between male FD patients and male stroke controls. [5] Another study has found a lower BA diameter cut-off of 2.98mm for all FD patients versus non-FD stroke controls (sensitivity 84% specificity 88.5%). [7] Since we had larger proportion of FD patients who suffered from stroke than other existing reports, we were able to conduct subgroup analysis on the predictive properties of BA diameter in both stroke and non-stroke categories. BA diameter of 4.16mm has a very high sensitivity and specificity to distinguish our subgroup of FD from matched stroke controls. As for FD without stroke, we also found a significant BA diameter cut-off value of 3.21mm with a sensitivity and specificity > 75%. These findings could assist physicians to decide whether to proceed for further FD diagnostic tests in stroke patients.
The BA cut-off values we obtained in our cohort of Chinese patients are bigger than the reported BA cut-off in other literature, probably due to inclusion of older FD patients especially patients with IVS4 variant. In fact, only 3 of our 10 FD stroke patients developed stroke at an age younger than 55. The five IVS4 patients who had stroke were between 65 to 72. Later-onset IVS4-type FD has long been considered as a cardiac variant, but studies in Taiwan have also shown that IVS4 patients have higher frequency of cerebral infarctions, pulvinar signs, and greater volume of WMH than general population. [15] Notably their BA diameter might even be larger than patients with classical FD. [16] Our study also demonstrated that FD patient with IVS4 mutation developed stroke at older age, they could be missed in most of the Fabry stroke screening programs where young stroke patients are targeted.
Though stroke is a common manifestation in FD, the stroke topography and exact stroke mechanism are unfortunately elusive. Among our ten patients who experienced stroke, each of them had more than one predisposing risk factors for stroke identified and the stroke etiology was diverse. Only one FD stroke patient did not have cardiomyopathy, while half of them had various degree of nephropathy. The proportion of cardiomyopathy among our cohort of Chinese FD patients was high, likely over-represented by the high prevalence of cardiac-variant IVS4 FD in our locality.
Another important finding of our study is the early onset of WMH among FD patients, in line with other existing data in which the surge of WMH burden started from the fourth decade and was earlier than the general population and patients with cerebrovascular diseases. [17,18]. The age of our cohort of Chinese FD patients was evenly distributed (eleven patients aged younger than 50, twelve patients aged between 50 and 64, and fourteen were at or above 65.) Only two patients did not have any WMH involvement, one-third (31.4%) had moderate CWML load with FAZEKAS score of at least 3. Among the young FD patients below 50, all patients had mild to moderate CWML involvement (FAZEKAS score 1–4). Particularly, our youngest patient also showed early WMH features at the age of 20, with punctate hyperintense foci present at the periventricular region. The two patients with the highest FAZEKAS score of 5 were in their fifties (aged 53 and 54). One of them was a IVS4 male patient who had serial MRIs performed. He already had mild bilateral microvascular ischaemic changes on his first MRI at the age of 46 and progressed to extensive white matter changes at the age of 54 despite treated with ERT and no known hypertension.
Although enzyme therapy becomes the standard of care in FD since 2001, its effect on cerebrovascular complications is seldom individually addressed. In a systematic review ERT appeared to decrease the stroke events, and another observational study from Japan suggested possible attenuation of BA diameter enlargement with ERT. [19,20] Nevertheless, the data is not conclusive and further data from longitudinal study is required for a better understanding on the influence of disease modifying therapies such as ERT or chaperon therapy on BA diameter and stroke occurrence.
Limitations
This study was limited by the retrospective design that the MRI technique was not standardized and we were unable to include the BA curved length, tortuosity index, laterality, and height of bifurcation in the measurements. We recommend full multimodal MRI and TOF-MRA imaging for better BA diameter measurements as BA sometimes extend obliquely and tortuously in which the largest cross-sectional diameter might not be observed at the mid-pons level.