Abstract
The discovery of biomarkers in rare diseases is of paramount importance to allow a better diagnosis, improve predictions of outcomes, and prompt the development of new treatments. Anti-N-methyl-D-aspartate receptor (NMDAR) encephalitis is a rare autoimmune disorder associated with the presence of antibodies targeting the GluN1 subunit of the NMDAR. Since it was discovered in 2007, large efforts have been made towards the identification of clinical, paraclinical, and molecular biomarkers to better understand the immune mechanisms that govern the course of the disease as well as to define predictors of treatment response and long-term outcomes. However, most of these biomarkers are still in an exploratory phase, with only a few candidates reaching the final phases of the always-complex process of biomarker development, mainly due to the low incidence of the disease and its recent description. Clinical and paraclinical markers are probably the most widely explored in anti-NMDAR encephalitis, five of them combined in a clinical score to predict 1 year outcome. On the contrary, soluble molecules, such as persistent antibody positivity, antibody titers, cytokines, and other inflammatory mediators, have been proposed as biomarkers of clinical activity, inflammation, prognosis, and treatment response, but further studies are required for their clinical validation including larger and more homogenous cohorts of patients. Similarly, genetic susceptibility biomarkers are still in the exploratory phase and, therefore, weak conclusions can for now only be achieved. Thus, further studies are warranted to define biomarkers and unravel the underlying mechanisms driving rare diseases such as anti-NMDAR encephalitis. Future international collaborative studies with prospective designs that enable the enrollment of large cohorts will allow for the identification and validation of novel biomarkers for clinical decision-making.
Highlights
We present an overview of the biomarkers described so far in antiNMDAR encephalitis, from clinical and paraclinical features identified during the routine diagnostic workup, to advanced molecular biomarkers that could improve our understanding of anti-N-methyl-D-aspartate receptor (NMDAR) encephalitis pathophysiology and lead to the development of novel targeted-treatments (Figure 1)
The development of biomarkers in rare disorders, such as anti-NMDAR encephalitis, may be challenging due to the difficulties related to collecting large cohorts of patients to achieve solid conclusions
The majority of biomarkers validated in anti-NMDAR encephalitis are clinical or paraclinical, whereas most soluble biomarkers are still at the early phases of their development, with the notable exception of cerebrospinal fluid (CSF) IgG NMDAR antibodies that have been widely implemented in clinical practice
Summary
In the evaluation process of a potential candidate, the general framework for developing disease-related biomarkers comprises different steps including biomarker discovery, analytical validation, qualification, and establishment of clinical utility [10] According to their applicability, biomarkers can be further classified as prognostic, susceptibility/risk, diagnostic, safety, monitoring, and predictive and treatmentresponse biomarkers [11]. No other biomarker is used for diagnostic, prognostic, monitoring, or therapeutic guidance besides clinical and paraclinical scores [12] Given this situation, the description of novel biomarkers in anti-NMDAR encephalitis is essential, especially to improve the current therapeutic management and to promote the development of new treatments that might accelerate recovery [2].
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