A human monoclonal antibody prevents malaria infection by targeting a new site of vulnerability on the parasite

Kisalu, Neville K.; Idris, Azza H.; Weidle, C.; Flores-García, Yevel; Flynn, Barbara J.; Sack, Brandon K.; Murphy, Sean C.; Schön, Arne; Freire, Ernesto; Francica, Joseph R.; Miller, Arnold; Gregory, J. Bancroft; March, Sandra; Liao, Hua Xin; Haynes, Barton F.; Wiehe, Kevin; Trama, Ashley M.; Saunders, Kevin O.; Gladden, Morgan A.; Monroe, Anthony; Bonsignori, Mattia; Kanekiyo, Masaru; Wheatley, Adam K.; McDermott, Adrian B.; Farney, S. Katie; Chuang, Gwo Yu; Zhang, Baoshan; Kc, Natasha; Chakravarty, Sumana; Kwong, Peter D.; Sinnis, Photini; Bhatia, Sangeeta N.; Kappe, Stefan H. I.; Sim, B. Kim Lee; Hoffman, Stephen L.; Zavala, Fidel; Pancera, Marie; Seder, Robert A.

doi:10.1038/nm.4512

Cited by 240 publications

(404 citation statements)

References 75 publications

(88 reference statements)

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“…All truncated PfCSPs in Imject® Alum conferred high protection (60%‐70%), indicating that all regions contribute to this protection. This result is consistent with other studies identifying protective human mAbs that potently bind to the “junctional” epitope between the N‐terminus and the central repeat of PfCSP . The present study demonstrated that PfCSP‐C immunization conferred protection and anti‐PfCSP‐C Abs reacted with the sporozoites.…”

Section: Discussionsupporting

confidence: 93%

“…Consistently, the present study revealed that anti‐repeat Abs had higher neutralizing activity in vitro than those of other regions. The superior action of anti‐repeat Abs may be attributable to their multivalent interactions and higher affinity of the repeat region . Therefore, the induction of the Ab titres by the repeat boost is the most potent and effective among the other truncated PfCSP‐boost immunizations against challenge by iv sporozoite injection.…”

Section: Discussionmentioning

confidence: 99%

“…However, in early studies, a NANP repeat‐based peptide‐in‐adjuvant vaccine failed to induce protective efficacy in field studies . Recently, Kisalu et al reported that a human monoclonal antibody (mAb) that recognizes a unique “junctional” epitope positioned between the N‐terminus and the central repeat region of PfCSP provided sterile protection against the bites of infected mosquitoes in a rodent malaria model. They suggested that this mAb inhibits not only sporozoite motility in the skin but also their invasion of hepatocytes by interfering with the cleavage of PfCSP.…”

Section: Introductionmentioning

confidence: 99%

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Down‐selecting circumsporozoite protein‐based malaria vaccine: A comparison of malaria sporozoite challenge model

Amelia

Iyori

Emran

et al. 2019

Parasite Immunology

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Summary Plasmodium falciparum circumsporozoite protein (PfCSP) is the main target antigen in development of pre‐erythrocytic malaria vaccines. To evaluate PfCSP vaccines in animal models, challenge by intravenous sporozoite injection is preferentially used. However, in clinical trials, vaccinated human volunteers are exposed to the bites of malaria‐infected mosquitoes. In this study, we down‐selected Escherichia coli‐produced full‐length PfCSP (PfCSP‐F) and its three truncated PfCSPs based on their abilities to elicit immune response and protection in mice against two challenge models. We showed that immunization with three doses of PfCSP‐F elicited high anti‐PfCSP antibody titres and 100% protection against the bites of infected mosquitoes. Meanwhile, three‐dose truncated PfCSP induced 60%‐70% protection after immunization with each truncated PfCSP. Heterologous prime‐boost immunization regimen with adenovirus‐PfCSP‐F and R32LR greatly induced complete protection against intravenous sporozoite injection. Our results suggest that Abs to both anti‐repeat and anti‐nonrepeat regions induced by PfCSP‐F are required to confer complete protection against challenge by the bites of infected mosquitoes, whereas anti‐repeat Abs play an important role in protection against intravenous sporozoite injection. Our findings provide a potential clinical application that PfCSP‐F vaccine induces potent Abs capable of neutralizing sporozoites in the dermis inoculated by infected mosquitoes and subsequently sporozoites in the blood circulation.

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Section: Discussionsupporting

confidence: 93%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Down‐selecting circumsporozoite protein‐based malaria vaccine: A comparison of malaria sporozoite challenge model

Amelia

Iyori

Emran

et al. 2019

Parasite Immunology

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“…Antibodies capable of neutralizing the pre‐erythrocytic sporozoite independent of complement can also prevent malaria infection in vitro and in vivo . For instance, one such antibody binds to and prevents the cleavage of the circumsporozoite protein, which is required for sporozoite infection of hepatocytes …”

mentioning

confidence: 99%

Immunoglobulin M, more than just an early responder to malaria

Boonyaratanakornkit

Taylor

2019

Immunol Cell Biol

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“…Recent studies have described mAbs CIS23, CIS34, CIS42 and CIS43 isolated from P. falciparum CSPspecific memory B-cells from volunteers who had been immunized with the PfSPZ vaccine [41][42][43]. CIS43 and MGG4 mAb had cross-reactivity with NPDP, NVDP and NANP repeat regions and the CTD fragment, thereby enabling them to bind to this protein and alter its cleavage after processing to limit hepatocyte invasion in an animal model [42][43][44]. The next step will involve clinical trials being run by PATH's Malaria Vaccine Initiative for determining whether mAbs can induce protection against P. falciparum infection.…”

Section: Genetically-attenuated Sporozoite Vaccinesmentioning

confidence: 99%

Plasmodium falciparum pre-erythrocytic stage vaccine development

Molina-Franky

Cuy-Chaparro

Camargo

et al. 2020

Malar J

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Worldwide strategies between 2010 and 2017 aimed at controlling malarial parasites (mainly Plasmodium falciparum) led to a reduction of just 18% regarding disease incidence rates. Many biologically-derived anti-malarial vaccine candidates have been developed to date; this has involved using many experimental animals, an immense amount of work and the investment of millions of dollars. This review provides an overview of the current state and the main results of clinical trials for sporozoite-targeting vaccines (i.e. the parasite stage infecting the liver) carried out by research groups in areas having variable malaria transmission rates. However, none has led to promising results regarding the effective control of the disease, thereby making it necessary to complement such efforts at finding/introducing new vaccine candidates by adopting a multi-epitope, multi-stage approach, based on minimal subunits of the main sporozoite proteins involved in the invasion of the liver.

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A human monoclonal antibody prevents malaria infection by targeting a new site of vulnerability on the parasite

Cited by 240 publications

References 75 publications

Down‐selecting circumsporozoite protein‐based malaria vaccine: A comparison of malaria sporozoite challenge model

Down‐selecting circumsporozoite protein‐based malaria vaccine: A comparison of malaria sporozoite challenge model

Immunoglobulin M, more than just an early responder to malaria

Plasmodium falciparum pre-erythrocytic stage vaccine development

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