Adsorptive depletion of blood monocytes reduces the levels of circulating interleukin-17A in Langerhans cell histiocytosis.

Langerhans cell histiocytosis (LCH) has been described as an inflammatory myeloid neoplasia that affects various organs. Central nervous system involvement may result in endocrinopathies and progressive neurodegeneration (ND-LCH), characterized by low-grade inflammation and degenerative changes, resulting in cognitive deficits, behavioral disturbances, and neuromotor dysfunction. Prolonged disease activity is a risk factor for ND-LCH. Potential biomarkers in cerebrospinal fluid (CSF) indicative of ND-LCH have been suggested (eg, neurofilament protein light chain [NF-L]), and increased interleukin-17A (IL-17A) levels in blood and extracranial lesions of LCH patients have been associated with local and systemic inflammation. Independently, IL-17A has been shown to disrupt the blood-brain barrier and increase production of reactive oxygen species in brain endothelial cells, pointing toward a crucial step for the development of experimental autoimmuneencephalitis andpossibly also for ND-LCH. There is currently no established therapy for ND-LCH, although many have been proposed. We aimed to find an effective therapy for a child with severe, rapidly progressive ND-LCH unresponsive to standard treatments. The patient was followed clinically (for .15 years), by magnetic resonance imaging (MRI) and bymeasuring NF-L in the CSF and later also IL-17A in CSF and plasma. Briefly, the patient was diagnosed with LCH at 5 months of age, which rapidly progressed into multisystem LCH with risk-organ involvement. Following initial treatment (LCH-II protocol) she stabilized, but after several reactivations, she developed a chronic active disease with elevated erythrocyte sedimentation rate (ESR). At 4 years of age, clinical signs ofNDwere noted (tripping, clumsiness), and brain MRI a year later revealed widespread ND-LCH affecting the basal ganglia, corpus callosum, cerebellum, and medulla. Despite many treatments, the patient deteriorated markedly within the next 4 years. Prompted by the need for effective treatment, at the age of 8 years we initiated granulocyte-and-monocyte apheresis (GMA), initially in parallel with conventional LCH treatment (Figure 1; at week 0), aiming at removing activated granulocytes and monocytes, thus reducing the inflammatory load. GMA was initially performed weekly for 10 weeks, followed by clinical improvement, decreased NF-L, and regression of cerebellar lesions. After a 10-week break, GMA was restarted and performed every second week (11 sessions). During a subsequent 4-month break, higher NF-L levels were noted, and GMA was restarted but performed less frequently and with fewer noticeable benefits. Therefore, her treatment was replaced with a combination of vinblastine and simvastatin (without GMA) to benefit from the antiinflammatory effect of simvastatin. However, the patient deteriorated the following 6 months with more fatigue, impaired balance and gait, and increased NF-L (Figure 1A). Nystagmus was confirmed a few months later. Given the positive effects of the first GMA treatments, GMA was restarted (week 115). Cytarabine was given in parallel for 6 months based on positive reports from others. Because of absence of clinical improvement and lack of alternative treatment, and considering the positive effects of natalizumab on patients with multiple sclerosis, we then administered natalizumab after thorough discussions with neurologists and the parents. GMA continued once every 4 weeks. Overall the patient tolerated the treatment well. After 6 months of natalizumab treatment, NF-L levels were lower, but at the 1-year follow-up, NF-L had increased again (Figure 1B; weeks 195 and 216, respectively), walking had deteriorated, and ESR indicated active inflammation (Figure 1A). Because of lack of improvement and increased risk of progressive multifocal leukoencephalopathy with prolonged treatment, natalizumab was ceased. Attracted by the lack of side effects from GMA in this patient who had not responded to other treatments, GMA was now (week 220) intensified to once weekly in parallel to low corticosteroid pulses (initially every 2 weeks, later every 3-4 weeks) for.2 years. NF-L decreased during this period, and the neurological deterioration eventually slowed down; the patient stabilized clinically, and MRI remained stable. In addition, but most apparent initially, positive effects were noted on the patient’s fatigue, possibly because of the marked decrease in circulating cytokine levels (Figure 1B-G). The impact of GMA over time on IL-17A in CSF, in plasma, and inside blood monocytes is illustrated in Figure 1B, C, and D, respectively. The methods used are described in the supplemental Materials and methods (available on the Blood Web site). When GMA was performed weekly, both the plasma IL-17A levels (Figure 1E) and the percentage of IL-17A monocytes in blood (Figure 1F) tended to be lower, compared with less frequent treatment, but the influence of spontaneous improvement or parallel treatments on this outcomecannot be ruled out.A remarkable reductionwas observed in IL-17A and IL-23 plasma levels during the last years (Figure 1G; week 326), whereas ESR remained slightly elevated. The increased IL-17A production on week 242 was accompanied by increased ESR and IL-23 levels, maybe because of subclinical infection. Stable low IL-17A plasma levels for the last 2 years and apparent neurological stabilization suggested less value from future GMA. Because of this and emerging difficulties with vascular access, GMA was stopped on