Multiple sclerosis in LRRK2 G2019S Parkinson’s disease and isolated nigral degeneration in a homozygous variant carrier

Adina Wise, Robert Ortega, D. Raymond, Alessandra Cervera, Emma Thorn, Katherine Leaver, David S. Russell, S. Bressman, J. Crary, R. Saunders-Pullman
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Abstract

LRRK2 variants have been associated with immune dysregulation as well as immune-related disorders such as IBD. A possible relationship between multiple sclerosis (MS) and LRRK2 PD has also been suggested. Further, neuropathologic studies of homozygous LRRK2 G2019S carriers with Parkinson’s disease (PD) are rare, and there are no systematic reports of clinical features in those cases.We investigated the co-occurrence of PD and MS in our research cohort and report on two cases of MS in LRRK2 PD as well as neuropathological findings for one.MS preceded PD in 1.4% (2/138) of participants with LRRK2 G2019S variants, and in none (0/638) with idiopathic PD (p = 0.03). One case with MS and PD was a LRRK2 G2019S homozygous carrier, and neuropathology showed evidence of substantia nigra pars compacta degeneration and pallor without Lewy deposition, as well as multiple white matter lesions consistent with MS-related demyelination.The increased prevalence of MS in LRRK2 PD further supports an important role for immune function for LRRK2 PD. This co-occurrence, while rare, suggests that MS may be an expression of the LRRK2 G2019S variant that includes both MS and PD, with MS predating features diagnostic of PD. The neuropathology suggests that the MS-related effects occurred independent of synuclein deposition. Importantly, and in addition, the neuropathological results not only support the MS diagnosis, but provide further evidence that Lewy body pathology may be absent even in homozygote LRRK2 carriers.
LRRK2 G2019S帕金森病中的多发性硬化症和同源变异携带者的孤立黑质变性
LRRK2 变异与免疫失调以及免疫相关疾病(如 IBD)有关。也有人认为多发性硬化症(MS)与 LRRK2 PD 之间可能存在关系。此外,针对帕金森病(PD)的同基因 LRRK2 G2019S 携带者的神经病理学研究非常罕见,也没有关于这些病例临床特征的系统报告。我们在研究队列中调查了帕金森病和多发性硬化症的并发情况,并报告了两例 LRRK2 帕金森病中的多发性硬化症病例以及其中一例的神经病理学发现。在患有 LRRK2 G2019S 变异的参与者中,有 1.4% (2/138)的人在帕金森病之前患有多发性硬化症,而在特发性帕金森病患者中,没有人(0/638)在帕金森病之前患有多发性硬化症(p = 0.03)。一例患有多发性硬化症和帕金森氏症的患者是 LRRK2 G2019S 基因同源携带者,神经病理学显示其黑质髓鞘变性和苍白,但无路易氏沉积,多处白质病变与多发性硬化症相关的脱髓鞘一致。这种并发症虽然罕见,但表明多发性硬化症可能是 LRRK2 G2019S 变体的一种表现形式,包括多发性硬化症和帕金森病,多发性硬化症早于帕金森病的诊断特征。神经病理学表明,与多发性硬化症相关的影响与突触核蛋白沉积无关。重要的是,此外,神经病理学结果不仅支持多发性硬化症的诊断,而且进一步证明了路易体病理学可能不存在于同型LRRK2携带者中。
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