Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation

Žilková, Monika; Nölle, Anna; Kováčech, Branislav; Kontseková, Eva; Weisová, Petronela; Filipčík, Peter; Škrabana, Rostislav; Prčina, Michal; Hromádka, Tomáš; Cehlár, Ondrej; Rolkova, Gabriela; Máderová, Denisa; Novák, Michal; Žilka, Norbert; Hoozemans, Jeroen J. M.

doi:10.1186/s40478-020-00948-z

Cited by 27 publications

(21 citation statements)

References 54 publications

(88 reference statements)

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“…Moreover, microglia are reported to have different regional abundance and activity states during aging, brain activity and neurodegenerative processes ( 58 , 70 – 72 ). In addition, accessing microglia in the human brain is in the majority of cases only possible in postmortem tissue ( 73 ).…”

Section: Discussionmentioning

confidence: 99%

Alzheimer’s Risk Gene TREM2 Determines Functional Properties of New Type of Human iPSC-Derived Microglia

et al. 2021

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Microglia are key in the homeostatic well-being of the brain and microglial dysfunction has been implicated in neurodegenerative disorders such as Alzheimer’s disease (AD). Due to the many limitations to study microglia in situ or isolated for large scale drug discovery applications, there is a high need to develop robust and scalable human cellular models of microglia with reliable translatability to the disease. Here, we describe the generation of microglia-like cells from human induced pluripotent stem cells (iPSC) with distinct phenotypes for mechanistic studies in AD. We started out from an established differentiation protocol to generate primitive macrophage precursors mimicking the yolk sac ontogeny of microglia. Subsequently, we tested 36 differentiation conditions for the cells in monoculture where we exposed them to various combinations of media, morphogens, and extracellular matrices. The optimized protocol generated robustly ramified cells expressing key microglial markers. Bulk mRNA sequencing expression profiles revealed that compared to cells obtained in co-culture with neurons, microglia-like cells derived from a monoculture condition upregulate mRNA levels for Triggering Receptor Expressed On Myeloid Cells 2 (TREM2), which is reminiscent to the previously described disease-associated microglia. TREM2 is a risk gene for AD and an important regulator of microglia. The regulatory function of TREM2 in these cells was confirmed by comparing wild type with isogenic TREM2 knock-out iPSC microglia. The TREM2-deficient cells presented with stronger increase in free cytosolic calcium upon stimulation with ATP and ADP, as well as stronger migration towards complement C5a, compared to TREM2 expressing cells. The functional differences were associated with gene expression modulation of key regulators of microglia. In conclusion, we have established and validated a work stream to generate functional human iPSC-derived microglia-like cells by applying a directed and neuronal co-culture independent differentiation towards functional phenotypes in the context of AD. These cells can now be applied to study AD-related disease settings and to perform compound screening and testing for drug discovery.

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Section: Discussionmentioning

confidence: 99%

Alzheimer’s Risk Gene TREM2 Determines Functional Properties of New Type of Human iPSC-Derived Microglia

et al. 2021

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“…Assuming that an effective therapeutic antibody should eliminate pathological tau proteins from the diseased brain, the effector function of such antibody becomes desirable. Our preclinical data with therapeutic anti-tau antibody AX004 indicate that IgG1 antibodies (with effector function) are more effective in facilitating the uptake of extracellular abnormal tau by adult human microglia than the IgG4 isotype (Zilkova et al 2020). Moreover, no safety signals have been observed throughout the course of the AADvac1 phase 1 and phase 2 clinical trials, although AADvac1 vaccination generated predominantly IgG1 antibody response in AD patients (Novak et al 2018).…”

Section: Discussionmentioning

confidence: 87%

“…This approach eliminates potential unfavourable effect of microglia activation but at the same time desirable tau clearing properties. In summary, tau-targeting vaccines recognize different tau species and have been suggested to act through various mechanisms: by preventing tau aggregation and cell-to-cell spreading (Theunis et al 2013;Albayram et al 2017;Courade et al 2018;Novak et al 2018;Albert et al 2019;Weisova et al 2019), by facilitating tau uptake by microglia (Zilkova et al 2020) and endo-lysosomal degradation of tau in microglia (Andersson et al 2019) or proteasomal degradation of tau seeds in neurons (McEwan et al 2017).…”

Section: The Role Of Microglia In Tau Immunotherapymentioning

confidence: 99%

“…Compelling body of evidence suggest that microglia engulf and degrade tau aggregates more efficiently in a complex with anti-tau antibody, which is an important underlying mechanism of action for the tau-targeted immunotherapy research. Various in vitro studies demonstrated how anti-tau antibodies significantly potentiate uptake and degradation of pathological tau via an Fc-dependent manner in BV2 microglia-like cells (Funk et al 2015), primary mouse microglia (Luo et al 2015;Andersson et al 2019) or primary human microglia (Zilkova et al 2020). Fc effector function is essential for the antibody-enhanced internalization and degradation of tau by microglia (Fig.…”

Section: Antibody-mediated Tau Clearance Might Alleviate Tau Pathologymentioning

confidence: 99%

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The engagement of microglia in tau-targeted immunotherapy in Alzheimer’s disease

Palova¹,

Csokova²,

Маркова³

et al. 2021

gpb

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Alzheimer's disease (AD) is an age-related neurodegenerative disease characterized by progressive memory decline, histopathological lesions such as amyloid β plaques and neurofibrillary tangles, and neuroinflammation driven by glial cells. Microglia, the innate immune cells of the brain, dynamically survey their environment for signs of infection and cell damage. Although our understanding of microglia and their modes of activation has expanded in recent years, their role in AD is still not completely understood. Broad range of microglia phenotypes, from neuroinflammatory to neuroprotective, found in neurodegenerative diseases make their role difficult to discern. In this review, we summarize activities of microglia in healthy and AD brains and their possible role during immunotherapy targeted against pathological tau proteins.

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“…When delivered with SUS +MB , RNF5 was only internalised into degenerating neurons and this is in line with other publications that have shown that antibodies are not readily internalised into neurons [25] or are only detected in dying neurons [27] which presents the possibility that RNF5 is acting in the extracellular space. Since we did not detect any increase in the phagocytic activity of the microglia in the RNF5-treated mice, we speculate that microglial phagocytosis may not be playing a significant role in tau clearance, despite being one of the well-documented mechanisms of action following passive immunotherapy with tau antibodies [20,21,28,29]. Alternatively, it may be possible that RNF5 is acting in the extracellular space to prevent the internalisation of tau seeds in the K3 mice, thus preventing the formation of insoluble tau species.…”

Section: Discussionmentioning

confidence: 99%

Ultrasound-mediated delivery of novel tau-specific monoclonal antibody enhances brain uptake but not therapeutic efficacy

Bajracharya

Cruz

Goetz

et al. 2021

Preprint

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Tau-specific immunotherapy is an attractive therapeutic strategy for the treatment of Alzheimer's disease and other tauopathies. However, targeting tau effectively remains a considerable challenge due to the restrictive nature of the blood-brain barrier (BBB), which excludes 99.9% of peripherally administered antibodies. We have previously shown that the delivery of tau-specific monoclonal antibody (mAb) with low-intensity scanning ultrasound in combination with intravenously injected microbubbles (SUS+MB) increases the passage of IgG antibodies into the brain. SUS+MB transiently opens tight junctions to allow paracellular transport, but also facilitates transcellular transport, particularly for larger cargoes. However, therapeutic efficacy after enhanced brain delivery has not been explored. To assess whether ultrasound-mediated delivery of tau-specific mAbs leads to an enhanced therapeutic response, K369I tau transgenic K3 mice were passively immunised once weekly for 12 weeks with a novel mAb, RNF5, in combination with SUS+MB. While none of the treatment arms improved behaviour or motor functions in these mice, we found that both RNF5 and SUS+MB treatments on their own reduced tau pathology, but, surprisingly, the combination of both (RNF5+SUS+MB) did not achieve an additive reduction in tau pathology. This was despite observing increased antibody penetration in the brain. Interestingly, a significant fraction of the antibody in the combination treatment was visualized in brain endothelial cells, suggesting that paracellular transport may not be the preferred uptake mechanism for RNF5. Taken altogether, more research is warranted to develop SUS+MB as a delivery modality for anti-tau antibodies.

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Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation

Cited by 27 publications

References 54 publications

Alzheimer’s Risk Gene TREM2 Determines Functional Properties of New Type of Human iPSC-Derived Microglia

Alzheimer’s Risk Gene TREM2 Determines Functional Properties of New Type of Human iPSC-Derived Microglia

The engagement of microglia in tau-targeted immunotherapy in Alzheimer’s disease

Ultrasound-mediated delivery of novel tau-specific monoclonal antibody enhances brain uptake but not therapeutic efficacy

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