Get It through Your Thick Head: Emerging Principles in Neuroimmunology and Neurovirology Redefine Central Nervous System “Immune Privilege”

Solomos, Andreas C.; Rall, Glenn F.

doi:10.1021/acschemneuro.5b00336

Cited by 21 publications

(16 citation statements)

References 65 publications

(109 reference statements)

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“…Our broadly mutated vaccine was also effective against gliomas in the immunologically distinct location of the brainstem [47][48][49] . The fact that anti-CTLA-4 improved vaccine efficacy in the B16 flank tumor model, but not in the GL261 intracranial model, is consistent with ICB therapy against brain tumors being limited by the ability of extracranially activated T cells to infiltrate into, and remain active in, the brain 50 .…”

Section: Discussionmentioning

confidence: 93%

APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy

et al. 2020

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APOBEC3B, an anti-viral cytidine deaminase which induces DNA mutations, has been implicated as a mediator of cancer evolution and therapeutic resistance. Mutational plasticity also drives generation of neoepitopes, which prime anti-tumor T cells. Here, we show that overexpression of APOBEC3B in tumors increases resistance to chemotherapy, but simultaneously heightens sensitivity to immune checkpoint blockade in a murine model of melanoma. However, in the vaccine setting, APOBEC3B-mediated mutations reproducibly generate heteroclitic neoepitopes in vaccine cells which activate de novo T cell responses. These cross react against parental, unmodified tumors and lead to a high rate of cures in both subcutaneous and intra-cranial tumor models. Heteroclitic Epitope Activated Therapy (HEAT) dispenses with the need to identify patient specific neoepitopes and tumor reactive T cells ex vivo. Thus, actively driving a high mutational load in tumor cell vaccines increases their immunogenicity to drive anti-tumor therapy in combination with immune checkpoint blockade.

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Section: Discussionmentioning

confidence: 93%

APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy

et al. 2020

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“…The healthy brain, while not usually patrolled directly by the adaptive immune system, is protected by a specialized cell type known as microglia [81]; microglia are bone marrow-derived innate immune cells that serve to protect the brain and maintain homeostasis [82, 83]. While microglia are normally a specialized brain-resident macrophage population [83], under pathological conditions such as inflammation [84], chronic stress [85], and radiation [86], bone marrow-derived myeloid progenitors can infiltrate the brain and differentiate into microglia-like cells.…”

Section: The Brain As a Unique Microenvironment For Metastasismentioning

confidence: 99%

Brain metastasis: Unique challenges and open opportunities

Lowery

2017

Biochimica et Biophysica Acta (BBA) - Reviews on Cancer

113

101

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The metastasis of cancer to the central nervous system (CNS) remains a devastating clinical reality, carrying an estimated survival time of less than one year in spite of recent therapeutic breakthroughs for other disease contexts. Advances in brain metastasis research are hindered by a number of reasons, including its complicated nature and the difficulty of modeling metastatic cancer growth in the unique brain microenvironment. In this review, we will discuss the clinical challenge, and compare the values and limitations of the available models for brain metastasis research. Additionally, we will specifically address current knowledge on how brain metastases take advantage of the unique brain environment to benefit their own growth. Finally, we will explore the distinctive metabolic and nutrient characteristics of the brain; how these paradoxically represent barriers to establishment of brain metastasis, but also provide ample supplies for metastatic cells’ growth in the brain. We envision that multi-disciplinary innovative approaches will open opportunities for the field to make breakthroughs in tackling unique challenges of brain metastasis.

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“…To support this development, microglia (resident macrophages in the CNS) identify infectious pathogens, plaques, and injured neurons; present them as antigens to T cells; and clear them through cytotoxicity, phagocytosis and synaptic stripping. Throughout development, then, while a highly coordinated series of peripheral immunologic events occurs, the developing CNS also requires constant immune homeostasis and surveillance, as well—in a manner that appears less ‘immune privileged’ than it is compartmentalized relative to peripheral blood [ 63 ].…”

Section: Introductionmentioning

confidence: 99%

Why monkeys do not get multiple sclerosis (spontaneously)

Bove

2018

Evolution, Medicine, and Public Health

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The goal of this review is to apply an evolutionary lens to understanding the origins of multiple sclerosis (MS), integrating three broad observations. First, only humans are known to develop MS spontaneously. Second, humans have evolved large brains, with characteristically large amounts of metabolically costly myelin. This myelin is generated over long periods of neurologic development—and peak MS onset coincides with the end of myelination. Third, over the past century there has been a disproportionate increase in the rate of MS in young women of childbearing age, paralleling increasing westernization and urbanization, indicating sexually specific susceptibility in response to changing exposures. From these three observations about MS, a life history approach leads us to hypothesize that MS arises in humans from disruption of the normal homeostatic mechanisms of myelin production and maintenance, during our uniquely long myelination period. This review will highlight under-explored areas of homeostasis in brain development, that are likely to shed new light on the origins of MS and to raise further questions about the interactions between our ancestral genes and modern environments.

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Get It through Your Thick Head: Emerging Principles in Neuroimmunology and Neurovirology Redefine Central Nervous System “Immune Privilege”

Cited by 21 publications

References 65 publications

APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy

APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy

Brain metastasis: Unique challenges and open opportunities

Why monkeys do not get multiple sclerosis (spontaneously)

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