In vivo imaging in NHP models of malaria: Challenges, progress and outlooks

Beignon, Anne-Sophie; Grand, Roger Le; Chapon, Catherine

doi:10.1016/j.parint.2013.09.001

Cited by 21 publications

(17 citation statements)

References 160 publications

(183 reference statements)

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“…NHP models could address problems involving metabolic and physiologic changes (eg, the pathogenesis of coma and neurologic dysfunction) that are difficult to study in human patients. 7 Functional magnetic resonance imaging, intracranial pressure monitoring, and laser video microscopy of flow and electroencephalogram under controlled settings (and in response to potential adjuvant therapies) are difficult to perform in human patients with malaria. In comparison with the nonsequestration-dependent, immune-mediated encephalitis of experimental murine cerebral malaria, the similarities of the pathophysiologic tapestry of P. coatneyi to human disease should make its results more medically relevant.…”

Section: Discussionmentioning

confidence: 99%

A Review of Plasmodium coatneyi–Macaque Models of Severe Malaria

et al. 2015

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Malaria remains one of the most significant public health concerns in the world today. Approximately half the human population is at risk for infection, with children and pregnant women being most vulnerable. More than 90% of the total human malaria burden, which numbers in excess of 200 million annually, is due to Plasmodium falciparum. Lack of an effective vaccine and a dwindling stockpile of antimalarial drugs due to increased plasmodial resistance underscore the critical need for valid animal models. Plasmodium coatneyi was described in Southeast Asia 50 years ago. This plasmodium of nonhuman primates has been used sporadically as a model for severe malaria, as it mimics many of the pathophysiologic features of human disease. This review covers the reported macroscopic, microscopic, ultrastructural, and molecular pathology of P. coatneyi infection in macaques, specifically focusing on the rhesus macaque, as well as describing the critical needs still outstanding in the validation of this crucial model of human disease.

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Section: Discussionmentioning

confidence: 99%

A Review of Plasmodium coatneyi–Macaque Models of Severe Malaria

et al. 2015

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“…the use of humanized mice in human malaria parasite Pe vaccine research P. falciparum and P. vivax PE stages exhibit a narrow host-cell tropism in which productive infection of host cells and complete liver-stage development is largely restricted to human and great ape hepatocytes [14]. This has been a significant hurdle for studying relevant liver-stage biology, immunology and vaccinology of these pathogens.…”

Section: Current Strategies To Identify and Validate Novel Pe Vaccine Tmentioning

confidence: 99%

“…Importantly, NHPs are the only model in which tissue-resident immune responses to human malaria parasite infection and vaccination can be assessed through tissue sampling, and NHP models have proven critical in P. vivax research [76]. NHP studies perhaps remain underutilized because of their significantly higher logistical, ethical and financial barriers, and while their immune systems more closely resemble that of humans, their more diverse histocompatibility complex loci could potentially misinform vaccine efficacy [75][76][77]. Furthermore, P. falciparum and P. vivax malaria parasites must be adapted to NHP models, a process that has been shown to result in altered parasite biology [72,78].…”

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confidence: 99%

“…Multi-epitope transgenic parasites have however recently been generated, and the advent of CRISPR/Cas9 usage in Plasmodium spp, may accelerate their creation by allowing direct replacement of essential genes without selection [73,82,83]. The predictive efficacy of the transgenic parasite screening approach remains unknown, and only once CHMI studies have been performed with antigens selected in this way will the utility of this model be determined definitively.the use of humanized mice in human malaria parasite Pe vaccine research P. falciparum and P. vivax PE stages exhibit a narrow host-cell tropism in which productive infection of host cells and complete liver-stage development is largely restricted to human and great ape hepatocytes [14]. This has been a significant hurdle for studying relevant liver-stage biology, immunology and vaccinology of these pathogens.…”

mentioning

confidence: 99%

“…In this perspective, we will explore how traditional animal models of malaria infection, in combination with in vitro assays, have contributed to the advancement of PE vaccine candidates to human clinical trials. While we acknowledge the critical contribution made by non-human primate (NHP) models of malaria [4,14], we focus on the role of small rodent models given their greater accessibility and cost-effectiveness early in vaccine discovery. Furthermore, malaria vaccine research has the advantage of a human challenge model known as controlled human malaria infection (CHMI).…”

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confidence: 99%

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An Expanding Toolkit for Preclinical Pre-Erythrocytic Malaria Vaccine Development: Bridging Traditional Mouse Malaria Models and Human Trials

2016

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Malaria remains a significant public health burden with 214 million new infections and over 400,000 deaths in 2015. Elucidating relevant Plasmodium parasite biology can lead to the identification of novel ways to control and ultimately eliminate the parasite within geographic areas. Particularly, the development of an effective vaccine that targets the clinically silent pre-erythrocytic stages of infection would significantly augment existing malaria elimination tools by preventing both the onset of blood-stage infection/disease as well as spread of the parasite through mosquito transmission. In this Perspective, we discuss the role of small animal models in pre-erythrocytic stage vaccine development, highlighting how human liver-chimeric and human immune system mice are emerging as valuable components of these efforts. Malaria continues to cause significant morbidity and mortality despite renewed and concerted efforts to eliminate the causative agents, parasites of the genus Plasmodium. These efforts have largely focused on control of the Anopheles mosquito vectors, and antimalarial drug treatment of symptomatic infected individuals. The 214 million new malaria infections and 438,000 deaths due to malaria in 2015 were disproportionately borne by low income countries where malaria is endemic, and declines in malaria infections since 2000 have been slowest in countries with low resource availability and high malaria burden [1]. In the fight against malaria, effective vaccines preventing both disease and transmission will be important tools to achieve WHO goals of a 90% reduction in disease burden by 2030 [1,2]. In humans, malaria is caused predominantly by the parasite species Plasmodium falciparum and Plasmodium vivax, with the remainder of infections caused by three additional parasite species, Plasmodium malariae, Plasmodium ovale and Plasmodium knowlesi [1].Malaria parasite transmission occurs when a Plasmodium-infected Anopheles mosquito bites and by probing the skin for a blood meal, deposits motile sporozoite stages into the host. Sporozoites pass through the dermis using active motility, enter a capillary and then rapidly home to the liver. Once in the liver sporozoites enter the parenchyma and infect hepatocytes, wherein they then transmogrify into liver stages, which grow, replicate and ultimately differentiate into tens of thousands of first-generation merozoites. Merozoites of human malaria parasites emerge from the liver into the blood stream 7-10 days after transmission, where they undergo cyclic erythrocytic infection and intraerythrocytic replication. This blood-stage infection is responsible for all mortality and clinical symptoms of malaria, as well as infection of a new mosquito vector by sexual stage parasites for onward transmission [3,4]. Stages prior to blood-stage infection (i.e., the sporozoite and liver stages) are collectively known as preerythrocytic (PE) stages of infection and vaccine candidates targeting these stages are collectively termed PE vaccines. By preventing progression to ...

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Animal Models of Infectious Diseases

Jena,

Pawar

2024

Animal Models in Research

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In vivo imaging in NHP models of malaria: Challenges, progress and outlooks

Cited by 21 publications

References 160 publications

A Review of Plasmodium coatneyi–Macaque Models of Severe Malaria

A Review of Plasmodium coatneyi–Macaque Models of Severe Malaria

An Expanding Toolkit for Preclinical Pre-Erythrocytic Malaria Vaccine Development: Bridging Traditional Mouse Malaria Models and Human Trials

Animal Models of Infectious Diseases

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