A Plasmodium falciparum 48/45 single epitope R0.6C subunit protein elicits high levels of transmission blocking antibodies

Susheel K Singh; Will Roeffen; Gorm Andersen; Teun Bousema; Michael Christiansen; Robert Sauerwein; Michael Theisen

doi:10.1016/j.vaccine.2015.02.040

A Plasmodium falciparum 48/45 single epitope R0.6C subunit protein elicits high levels of transmission blocking antibodies

Susheel K Singh, Will Roeffen, Gorm Andersen, Teun Bousema, Michael Christiansen, Robert Sauerwein, Michael Theisen

37 Citationer (Scopus)

Abstract

The sexual stage Pfs48/45 antigen is a well-established lead candidate for a transmission blocking (TB) vaccine because of its critical role in parasite fertilization. We have recently produced the carboxy-terminal 10C-fragment of Pfs48/45 containing three known epitopes for TB antibodies as a chimera with the N-terminal region of GLURP (R0). The resulting fusion protein elicited high titer TB antibodies in rodents. To increase the relatively low yield of correctly folded Pfs48/45 we have generated a series of novel chimera truncating the 10C-fragments to 6 cysteine residues containing sub-units (6C). All constructs harbor the major epitope I for TB antibodies. One of these sub-units (R0.6Cc), produced high yields of correctly folded conformers, which could be purified by a simple 2-step procedure. Purified R0.6Cc was stable and elicits high titer TB antibodies in rats. The yield, purity and stability of R0.6Cc allows for further clinical development.

Originalsprog	Engelsk
Tidsskrift	Vaccine
Vol/bind	33
Udgave nummer	16
Sider (fra-til)	1981-6
Antal sider	6
ISSN	0264-410X
DOI	https://doi.org/10.1016/j.vaccine.2015.02.040
Status	Udgivet - 15 apr. 2015

FN’s Verdensmål

Dette resultat bidrager til følgende verdensmål

Adgang til dokumentet

10.1016/j.vaccine.2015.02.040

Citationsformater

@article{f343309a557541d7bfb146d2b4a7c92e,

title = "A Plasmodium falciparum 48/45 single epitope R0.6C subunit protein elicits high levels of transmission blocking antibodies",

abstract = "The sexual stage Pfs48/45 antigen is a well-established lead candidate for a transmission blocking (TB) vaccine because of its critical role in parasite fertilization. We have recently produced the carboxy-terminal 10C-fragment of Pfs48/45 containing three known epitopes for TB antibodies as a chimera with the N-terminal region of GLURP (R0). The resulting fusion protein elicited high titer TB antibodies in rodents. To increase the relatively low yield of correctly folded Pfs48/45 we have generated a series of novel chimera truncating the 10C-fragments to 6 cysteine residues containing sub-units (6C). All constructs harbor the major epitope I for TB antibodies. One of these sub-units (R0.6Cc), produced high yields of correctly folded conformers, which could be purified by a simple 2-step procedure. Purified R0.6Cc was stable and elicits high titer TB antibodies in rats. The yield, purity and stability of R0.6Cc allows for further clinical development.",

author = "Singh, {Susheel K} and Will Roeffen and Gorm Andersen and Teun Bousema and Michael Christiansen and Robert Sauerwein and Michael Theisen",

year = "2015",

month = apr,

day = "15",

doi = "10.1016/j.vaccine.2015.02.040",

language = "English",

volume = "33",

pages = "1981--6",

journal = "Vaccine",

issn = "0264-410X",

publisher = "Elsevier",

number = "16",

}

TY - JOUR

T1 - A Plasmodium falciparum 48/45 single epitope R0.6C subunit protein elicits high levels of transmission blocking antibodies

AU - Singh, Susheel K

AU - Roeffen, Will

AU - Andersen, Gorm

AU - Bousema, Teun

AU - Christiansen, Michael

AU - Sauerwein, Robert

AU - Theisen, Michael

PY - 2015/4/15

Y1 - 2015/4/15

N2 - The sexual stage Pfs48/45 antigen is a well-established lead candidate for a transmission blocking (TB) vaccine because of its critical role in parasite fertilization. We have recently produced the carboxy-terminal 10C-fragment of Pfs48/45 containing three known epitopes for TB antibodies as a chimera with the N-terminal region of GLURP (R0). The resulting fusion protein elicited high titer TB antibodies in rodents. To increase the relatively low yield of correctly folded Pfs48/45 we have generated a series of novel chimera truncating the 10C-fragments to 6 cysteine residues containing sub-units (6C). All constructs harbor the major epitope I for TB antibodies. One of these sub-units (R0.6Cc), produced high yields of correctly folded conformers, which could be purified by a simple 2-step procedure. Purified R0.6Cc was stable and elicits high titer TB antibodies in rats. The yield, purity and stability of R0.6Cc allows for further clinical development.

AB - The sexual stage Pfs48/45 antigen is a well-established lead candidate for a transmission blocking (TB) vaccine because of its critical role in parasite fertilization. We have recently produced the carboxy-terminal 10C-fragment of Pfs48/45 containing three known epitopes for TB antibodies as a chimera with the N-terminal region of GLURP (R0). The resulting fusion protein elicited high titer TB antibodies in rodents. To increase the relatively low yield of correctly folded Pfs48/45 we have generated a series of novel chimera truncating the 10C-fragments to 6 cysteine residues containing sub-units (6C). All constructs harbor the major epitope I for TB antibodies. One of these sub-units (R0.6Cc), produced high yields of correctly folded conformers, which could be purified by a simple 2-step procedure. Purified R0.6Cc was stable and elicits high titer TB antibodies in rats. The yield, purity and stability of R0.6Cc allows for further clinical development.

U2 - 10.1016/j.vaccine.2015.02.040

DO - 10.1016/j.vaccine.2015.02.040

M3 - Journal article

C2 - 25728318

SN - 0264-410X

VL - 33

SP - 1981

EP - 1986

JO - Vaccine

JF - Vaccine

IS - 16

ER -

A Plasmodium falciparum 48/45 single epitope R0.6C subunit protein elicits high levels of transmission blocking antibodies

Abstract

FN’s Verdensmål

Adgang til dokumentet

Fingeraftryk

Citationsformater