Your search keyword '"PfCSP"' showing total 12 results

1. Plasmodium falciparum AMA1 and CSP antigen diversity in parasite isolates from southern Ghana.

Author

Kusi, Kwadwo A., Amoah, Linda E., Kojo Acquah, Festus, Ennuson, Nana Aba, Frempong, Abena F., Ofori, Ebenezer A., Akyea-Mensah, Kwadwo, Kyei-Baafour, Eric, Osei, Frank, Frimpong, Augustina, Singh, Susheel K., Theisen, Michael, Remarque, Edmond J., Faber, Bart W., Belmonte, Maria, Ganeshan, Harini, Jun Huang, Villasante, Eileen, and Sedegah, Martha

Subjects

PARASITE antigens, PLASMODIUM, PLASMODIUM falciparum, CIRCUMSPOROZOITE protein, SINGLE nucleotide polymorphisms, PEPTIDOMIMETICS, ANTIBODY formation, IMMUNOGLOBULINS

Abstract

Introduction: Diversity in malarial antigens is an immune evasion mechanism that gives malaria parasites an edge over the host. Immune responses against one variant of a polymorphic antigen are usually not fully effective against other variants due to altered epitopes. This study aimed to evaluate diversity in the Plasmodium falciparum antigens apical membrane antigen 1 (PfAMA1) and circumsporozoite protein (PfCSP) from circulating parasites in a malaria-endemic community in southern Ghana and to determine the effects of polymorphisms on antibody response specificity. Methods: The study involved 300 subjects, whose P. falciparum infection status was determined by microscopy and PCR. Diversity within the two antigens was evaluated by msp2 gene typing and molecular gene sequencing, while the host plasma levels of antibodies against PfAMA1, PfCSP, and two synthetic 24mer peptides from the conserved central repeat region of PfCSP, were measured by ELISA. Results: Of the 300 subjects, 171 (57%) had P. falciparum infection, with 165 of the 171 (96.5%) being positive for either or both of the msp2 allelic families. Gene sequencing of DNA from 55 clonally infected samples identified a total of 56 non-synonymous single nucleotide polymorphisms (SNPs) for the Pfama1 gene and these resulted in 44 polymorphic positions, including two novel positions (363 and 365). Sequencing of the Pfcsp gene from 69 clonal DNA samples identified 50 non-synonymous SNPs that resulted in 42 polymorphic positions, with half (21) of these polymorphic positions being novel. Of the measured antibodies, only anti-PfCSP antibodies varied considerably between PCR parasite-positive and parasite-negative persons. Discussion: These data confirm the presence of a considerable amount of unique, previously unreported amino acid changes, especially within PfCSP. Drivers for this diversity in the Pfcsp gene do not immediately seem apparent, as immune pressure will be expected to drive a similar level of diversity in the Pfamal gene. [ABSTRACT FROM AUTHOR]

Published

2024

2. Plasmodium falciparum AMA1 and CSP antigen diversity in parasite isolates from southern Ghana

Author

Kwadwo A. Kusi, Linda E. Amoah, Festus Kojo Acquah, Nana Aba Ennuson, Abena F. Frempong, Ebenezer A. Ofori, Kwadwo Akyea-Mensah, Eric Kyei-Baafour, Frank Osei, Augustina Frimpong, Susheel K. Singh, Michael Theisen, Edmond J. Remarque, Bart W. Faber, Maria Belmonte, Harini Ganeshan, Jun Huang, Eileen Villasante, and Martha Sedegah

Subjects

polymorphism, Ghana, plasmodium, malaria, PfAMA1, PFCSP, Microbiology, QR1-502

Abstract

IntroductionDiversity in malarial antigens is an immune evasion mechanism that gives malaria parasites an edge over the host. Immune responses against one variant of a polymorphic antigen are usually not fully effective against other variants due to altered epitopes. This study aimed to evaluate diversity in the Plasmodium falciparum antigens apical membrane antigen 1 (PfAMA1) and circumsporozoite protein (PfCSP) from circulating parasites in a malaria-endemic community in southern Ghana and to determine the effects of polymorphisms on antibody response specificity.MethodsThe study involved 300 subjects, whose P. falciparum infection status was determined by microscopy and PCR. Diversity within the two antigens was evaluated by msp2 gene typing and molecular gene sequencing, while the host plasma levels of antibodies against PfAMA1, PfCSP, and two synthetic 24mer peptides from the conserved central repeat region of PfCSP, were measured by ELISA. ResultsOf the 300 subjects, 171 (57%) had P. falciparum infection, with 165 of the 171 (96.5%) being positive for either or both of the msp2 allelic families. Gene sequencing of DNA from 55 clonally infected samples identified a total of 56 non-synonymous single nucleotide polymorphisms (SNPs) for the Pfama1 gene and these resulted in 44 polymorphic positions, including two novel positions (363 and 365). Sequencing of the Pfcsp gene from 69 clonal DNA samples identified 50 non-synonymous SNPs that resulted in 42 polymorphic positions, with half (21) of these polymorphic positions being novel. Of the measured antibodies, only anti-PfCSP antibodies varied considerably between PCR parasite-positive and parasite-negative persons. DiscussionThese data confirm the presence of a considerable amount of unique, previously unreported amino acid changes, especially within PfCSP. Drivers for this diversity in the Pfcsp gene do not immediately seem apparent, as immune pressure will be expected to drive a similar level of diversity in the Pfama1 gene.

Published

2024

3. Molecular and functional properties of human Plasmodium falciparum CSP C‐terminus antibodies

Author

Opeyemi Ernest Oludada, Giulia Costa, Clare Burn Aschner, Anna S Obraztsova, Katherine Prieto, Caterina Canetta, Stephen L Hoffman, Peter G Kremsner, Benjamin Mordmüller, Rajagopal Murugan, Jean‐Philippe Julien, Elena A Levashina, and Hedda Wardemann

Subjects

Affinity maturation, Antibodies, Malaria, PfCSP, Plasmodium, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Human monoclonal antibodies (mAbs) against the central repeat and junction domain of Plasmodium falciparum circumsporozoite protein (PfCSP) have been studied extensively to guide malaria vaccine design compared to antibodies against the PfCSP C terminus. Here, we describe the molecular characteristics and protective potential of 73 germline and mutated human mAbs against the highly immunogenic PfCSP C‐terminal domain. Two mAbs recognized linear epitopes in the C‐terminal linker with sequence similarity to repeat and junction motifs, whereas all others targeted conformational epitopes in the α‐thrombospondin repeat (α‐TSR) domain. Specificity for the polymorphic Th2R/Th3R but not the conserved RII+/CS.T3 region in the α‐TSR was associated with IGHV3‐21/IGVL3‐21 or IGLV3‐1 gene usage. Although the C terminus specific mAbs showed signs of more efficient affinity maturation and class‐switching compared to anti‐repeat mAbs, live sporozoite binding and inhibitory activity was limited to a single C‐linker reactive mAb with cross‐reactivity to the central repeat and junction. The data provide novel insights in the human anti‐C‐linker and anti‐α‐TSR antibody response that support exclusion of the PfCSP C terminus from malaria vaccine designs.

Published

2023

4. Molecular and functional properties of human Plasmodium falciparum CSP C‐terminus antibodies.

Author

Oludada, Opeyemi Ernest, Costa, Giulia, Burn Aschner, Clare, Obraztsova, Anna S, Prieto, Katherine, Canetta, Caterina, Hoffman, Stephen L, Kremsner, Peter G, Mordmüller, Benjamin, Murugan, Rajagopal, Julien, Jean‐Philippe, Levashina, Elena A, and Wardemann, Hedda

Abstract

Human monoclonal antibodies (mAbs) against the central repeat and junction domain of Plasmodium falciparum circumsporozoite protein (PfCSP) have been studied extensively to guide malaria vaccine design compared to antibodies against the PfCSP C terminus. Here, we describe the molecular characteristics and protective potential of 73 germline and mutated human mAbs against the highly immunogenic PfCSP C‐terminal domain. Two mAbs recognized linear epitopes in the C‐terminal linker with sequence similarity to repeat and junction motifs, whereas all others targeted conformational epitopes in the α‐thrombospondin repeat (α‐TSR) domain. Specificity for the polymorphic Th2R/Th3R but not the conserved RII+/CS.T3 region in the α‐TSR was associated with IGHV3‐21/IGVL3‐21 or IGLV3‐1 gene usage. Although the C terminus specific mAbs showed signs of more efficient affinity maturation and class‐switching compared to anti‐repeat mAbs, live sporozoite binding and inhibitory activity was limited to a single C‐linker reactive mAb with cross‐reactivity to the central repeat and junction. The data provide novel insights in the human anti‐C‐linker and anti‐α‐TSR antibody response that support exclusion of the PfCSP C terminus from malaria vaccine designs. Synopsis: Plasmodium falciparum circumsporozoite protein (PfCSP) is a promising malaria vaccine target. Antibodies against the PfCSP central repeat domain and N‐terminal junction mediate protection from the infection, but the role of antibodies against the C‐terminal domain (C‐CSP) remains controversial. High‐affinity human C‐CSP antibodies failed to bind live P. falciparum sporozoites and lacked parasite‐inhibitory activity at 100‐fold higher concentration than repeat antibodies or antibodies with C‐CSP and repeat/junction cross‐reactivity.IGHV3‐21 gene usage was linked to antibodies that bound polymorphic epitopes in the α‐TSR subdomain of recombinant C‐CSP, whereas rare antibodies against conserved α‐TSR epitopes were encoded by diverse genes.IGHV3‐21‐encoded C‐CSP‐reactive antibodies showed signs of more efficient affinity maturation than IGHV3‐33‐encoded anti‐repeat/junction antibodies.Crystal structure and molecular modeling help to explain the C‐CSP specificity of a unique IGHV3‐33‐encoded antibody against a linear epitope in the C‐linker with sequence similarity to the repeat/junction. [ABSTRACT FROM AUTHOR]

Published

2023

5. Increased levels of anti-PfCSP antibodies in post-pubertal females versus males immunized with PfSPZ Vaccine does not translate into increased protective efficacy.

Author

KC, Natasha, Preston Church, L. W., Riyahi, Pouria, Chakravarty, Sumana, Seder, Robert A., Epstein, Judith E., Lyke, Kirsten E., Mordmüller, Benjamin, Kremsner, Peter G., Sissoko, Mahamadou S., Healy, Sarah, Duffy, Patrick E., Jongo, Said A., Nsue Ndong Nchama, Vicente Urbano, Abdulla, Salim, Mpina, Maxmillian, Sirima, Sodiomon B., Laurens, Matthew B., Steinhardt, Laura C., and Oneko, Martina

Subjects

MALARIA vaccines, DEVELOPMENTAL biology, IMMUNOGLOBULINS, CIRCUMSPOROZOITE protein, ENZYME-linked immunosorbent assay, HUMORAL immunity, HERD immunity

Abstract

Background: While prior research has shown differences in the risk of malaria infection and sickness between males and females, little is known about sex differences in vaccine-induced immunity to malaria. Identifying such differences could elucidate important aspects of malaria biology and facilitate development of improved approaches to malaria vaccination. Methods: Using a standardized enzyme-linked immunosorbent assay, IgG antibodies to the major surface protein on Plasmodium falciparum (Pf) sporozoites (SPZ), the Pf circumsporozoite protein (PfCSP), were measured before and two weeks after administration of a PfSPZ-based malaria vaccine (PfSPZ Vaccine) to 5-month to 61-year-olds in 11 clinical trials in Germany, the US and five countries in Africa, to determine if there were differences in vaccine elicited antibody response between males and females and if these differences were associated with differential protection against naturally transmitted Pf malaria (Africa) or controlled human malaria infection (Germany, the US and Africa). Results: Females ≥ 11 years of age made significantly higher levels of antibodies to PfCSP than did males in most trials, while there was no indication of such differences in infants or children. Although adult females had higher levels of antibodies, there was no evidence of improved protection compared to males. In 2 of the 7 trials with sufficient data, protected males had significantly higher levels of antibodies than unprotected males, and in 3 other trials protected females had higher levels of antibodies than did unprotected females. Conclusion: Immunization with PfSPZ Vaccine induced higher levels of antibodies in post-pubertal females but showed equivalent protection in males and females. We conclude that the increased antibody levels in postpubertal females did not contribute substantially to improved protection. We hypothesize that while antibodies to PfCSP (and PfSPZ) may potentially contribute directly to protection, they primarily correlate with other, potentially protective immune mechanisms, such as antibody dependent and antibody independent cellular responses in the liver. [ABSTRACT FROM AUTHOR]

Published

2022

6. Increased levels of anti-PfCSP antibodies in post-pubertal females versus males immunized with PfSPZ Vaccine does not translate into increased protective efficacy

Author

Natasha KC, L. W. Preston Church, Pouria Riyahi, Sumana Chakravarty, Robert A. Seder, Judith E. Epstein, Kirsten E. Lyke, Benjamin Mordmüller, Peter G. Kremsner, Mahamadou S. Sissoko, Sara Healy, Patrick E. Duffy, Said A. Jongo, Vicente Urbano Nsue Ndong Nchama, Salim Abdulla, Maxmillian Mpina, Sodiomon B. Sirima, Matthew B. Laurens, Laura C. Steinhardt, Martina Oneko, MingLin Li, Tooba Murshedkar, Peter F. Billingsley, B. Kim Lee Sim, Thomas L. Richie, and Stephen L. Hoffman

Subjects

PfSPZ Vaccine, malaria vaccine, Plasmodium falciparum, PfCSP, antibodies, humoral immunity, Immunologic diseases. Allergy, RC581-607

Abstract

BackgroundWhile prior research has shown differences in the risk of malaria infection and sickness between males and females, little is known about sex differences in vaccine-induced immunity to malaria. Identifying such differences could elucidate important aspects of malaria biology and facilitate development of improved approaches to malaria vaccination.MethodsUsing a standardized enzyme-linked immunosorbent assay, IgG antibodies to the major surface protein on Plasmodium falciparum (Pf) sporozoites (SPZ), the Pf circumsporozoite protein (PfCSP), were measured before and two weeks after administration of a PfSPZ-based malaria vaccine (PfSPZ Vaccine) to 5-month to 61-year-olds in 11 clinical trials in Germany, the US and five countries in Africa, to determine if there were differences in vaccine elicited antibody response between males and females and if these differences were associated with differential protection against naturally transmitted Pf malaria (Africa) or controlled human malaria infection (Germany, the US and Africa).ResultsFemales ≥ 11 years of age made significantly higher levels of antibodies to PfCSP than did males in most trials, while there was no indication of such differences in infants or children. Although adult females had higher levels of antibodies, there was no evidence of improved protection compared to males. In 2 of the 7 trials with sufficient data, protected males had significantly higher levels of antibodies than unprotected males, and in 3 other trials protected females had higher levels of antibodies than did unprotected females.ConclusionImmunization with PfSPZ Vaccine induced higher levels of antibodies in post-pubertal females but showed equivalent protection in males and females. We conclude that the increased antibody levels in post-pubertal females did not contribute substantially to improved protection. We hypothesize that while antibodies to PfCSP (and PfSPZ) may potentially contribute directly to protection, they primarily correlate with other, potentially protective immune mechanisms, such as antibody dependent and antibody independent cellular responses in the liver.

Published

2022

7. Sterile protection and transmission blockade by a multistage anti-malarial vaccine in the pre-clinical study.

Author

Mitsuhiro Iyori, Blagborough, Andrew M., Tetsushi Mizuno, Yu-ichi Abe, Mio Nagaoka, Naoto Hori, Iroha Yamagoshi, Da, Dari F., Gregory, William F., Hasyim, Ammar A., Yutaro Yamamoto, Akihiko Sakamoto, Kunitaka Yoshida, Hiroaki Mizukami, Hisatoshi Shida, and Shigeto Yoshida

Subjects

MALARIA vaccines, SMALLPOX vaccines, CIRCUMSPOROZOITE protein, VACCINIA, GENETIC vectors

Abstract

The Malaria Vaccine Technology Roadmap 2013 (World Health Organization) aims to develop safe and effective vaccines by 2030 that will offer at least 75% protective efficacy against clinical malaria and reduce parasite transmission. Here, we demonstrate a highly effective multistage vaccine against both the pre-erythrocytic and sexual stages of Plasmodium falciparum that protects and reduces transmission in a murine model. The vaccine is based on a viral-vectored vaccine platform, comprising a highly-attenuated vaccinia virus strain, LC16m8Δ (m8Δ), a genetically stable variant of a licensed and highly effective Japanese smallpox vaccine LC16m8, and an adeno-associated virus (AAV), a viral vector for human gene therapy. The genes encoding P. falciparum circumsporozoite protein (PfCSP) and the ookinete protein P25 (Pfs25) are expressed as a Pfs25–PfCSP fusion protein, and the heterologous m8Δ-prime/AAV-boost immunization regimen in mice provided both 100% protection against PfCSP-transgenic P. berghei sporozoites and up to 100% transmission blocking efficacy, as determined by a direct membrane feeding assay using parasites from P. falciparum-positive, naturally-infected donors from endemic settings. Remarkably, the persistence of vaccine-induced immune responses were over 7 months and additionally provided complete protection against repeated parasite challenge in a murine model. We propose that application of the m8Δ/AAV malaria multistage vaccine platform has the potential to contribute to the landmark goals of the malaria vaccine technology roadmap, to achieve life-long sterile protection and high-level transmission blocking efficacy. [ABSTRACT FROM AUTHOR]

Published

2022

8. Expanding the Malaria Antibody Toolkit: Development and Characterisation of Plasmodium falciparum RH5, CyRPA, and CSP Recombinant Human Monoclonal Antibodies.

Author

Nacer, Adéla, Kivi, Gaily, Pert, Raini, Juronen, Erkki, Holenya, Pavlo, Aliprandini, Eduardo, Amino, Rogerio, Silvie, Olivier, Quinkert, Doris, Le Duff, Yann, Hurley, Matthew, Reimer, Ulf, Tover, Andres, Draper, Simon J., Gilbert, Sarah, Ho, Mei Mei, and Bowyer, Paul W.

Subjects

MALARIA, PLASMODIUM falciparum, RECOMBINANT antibodies, CIRCUMSPOROZOITE protein, CARRIER proteins, IMMUNOGLOBULINS, MONOCLONAL antibodies

Abstract

Malaria, an infection caused by apicomplexan parasites of the genus Plasmodium , continues to exact a significant toll on public health with over 200 million cases world-wide, and annual deaths in excess of 600,000. Considerable progress has been made to reduce malaria burden in endemic countries in the last two decades. However, parasite and mosquito resistance to frontline chemotherapies and insecticides, respectively, highlights the continuing need for the development of safe and effective vaccines. Here we describe the development of recombinant human antibodies to three target proteins from Plasmodium falciparum : reticulocyte binding protein homologue 5 (PfRH5), cysteine-rich protective antigen (Pf CyRPA), and circumsporozoite protein (Pf CSP). All three proteins are key targets in the development of vaccines for blood-stage or pre-erythrocytic stage infections. We have developed potent anti- Pf RH5, Pf CyRPA and Pf CSP monoclonal antibodies that will prove useful tools for the standardisation of assays in preclinical research and the assessment of these antigens in clinical trials. We have generated some very potent anti- Pf RH5 and anti- Pf CyRPA antibodies with some clones >200 times more potent than the polyclonal anti-AMA-1 antibodies used for the evaluation of blood stage antigens. While the monoclonal and polyclonal antibodies are not directly comparable, the data provide evidence that these new antibodies are very good at blocking invasion. These antibodies will therefore provide a valuable resource and have potential as biological standards to help harmonise pre-clinical malaria research. [ABSTRACT FROM AUTHOR]

Published

2022

9. Sterile protection and transmission blockade by a multistage anti-malarial vaccine in the pre-clinical study.

Author

Iyori M, Blagborough AM, Mizuno T, Abe YI, Nagaoka M, Hori N, Yamagoshi I, Da DF, Gregory WF, Hasyim AA, Yamamoto Y, Sakamoto A, Yoshida K, Mizukami H, Shida H, and Yoshida S

Subjects

Animals, Antibodies, Protozoan, Dependovirus genetics, Disease Models, Animal, Humans, Mice, Protozoan Proteins genetics, Antimalarials, Malaria Vaccines, Malaria, Falciparum

Abstract

The Malaria Vaccine Technology Roadmap 2013 (World Health Organization) aims to develop safe and effective vaccines by 2030 that will offer at least 75% protective efficacy against clinical malaria and reduce parasite transmission. Here, we demonstrate a highly effective multistage vaccine against both the pre-erythrocytic and sexual stages of Plasmodium falciparum that protects and reduces transmission in a murine model. The vaccine is based on a viral-vectored vaccine platform, comprising a highly-attenuated vaccinia virus strain, LC16m8Δ (m8Δ), a genetically stable variant of a licensed and highly effective Japanese smallpox vaccine LC16m8, and an adeno-associated virus (AAV), a viral vector for human gene therapy. The genes encoding P. falciparum circumsporozoite protein (PfCSP) and the ookinete protein P25 (Pfs25) are expressed as a Pfs25-PfCSP fusion protein, and the heterologous m8Δ-prime/AAV-boost immunization regimen in mice provided both 100% protection against PfCSP-transgenic P. berghei sporozoites and up to 100% transmission blocking efficacy, as determined by a direct membrane feeding assay using parasites from P. falciparum -positive, naturally-infected donors from endemic settings. Remarkably, the persistence of vaccine-induced immune responses were over 7 months and additionally provided complete protection against repeated parasite challenge in a murine model. We propose that application of the m8Δ/AAV malaria multistage vaccine platform has the potential to contribute to the landmark goals of the malaria vaccine technology roadmap, to achieve life-long sterile protection and high-level transmission blocking efficacy., Competing Interests: The authors have read the journal’s policy and declare the following conflicts of interest: Authors SY, HS, HM and MI are named inventors on filed patents related to viral-vectored malaria vaccines (2022-24221). HS is a named inventor on a filed patent related to LC16m8Δ (WO 2005/054451 A1). Neither of these products has been commercialized. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Iyori, Blagborough, Mizuno, Abe, Nagaoka, Hori, Yamagoshi, Da, Gregory, Hasyim, Yamamoto, Sakamoto, Yoshida, Mizukami, Shida and Yoshida.)

Published

2022

10. Schur-concave triangular norms: Characterization and application in pFCSP

Author

Takači, Aleksandar

Subjects

*CONCAVE functions, *MATRIX norms, *REAL variables, *FUZZY sets

Abstract

Abstract: The concept of priority is often used in real time systems. Schur-concave t-norms are used to capture this concept within prioritized fuzzy constraint satisfaction problems (pFCSPs). We are dealing with a very strict notion of priority which favors the constraint with the larger priority regardless of its value.Also, some results on the characterization of Schur-concave t-norms are given. [Copyright &y& Elsevier]

Published

2005

11. Vaccination in a humanized mouse model elicits highly protective PfCSP-targeting anti-malarial antibodies.

Author

Kratochvil, Sven, Shen, Chen-Hsiang, Lin, Ying-Cing, Xu, Kai, Nair, Usha, Da Silva Pereira, Lais, Tripathi, Prabhanshu, Arnold, Johan, Chuang, Gwo-Yu, Melzi, Eleonora, Schön, Arne, Zhang, Baoshan, Dillon, Marlon, Bonilla, Brian, Flynn, Barbara J., Kirsch, Kathrin H., Kisalu, Neville K., Kiyuka, Patience K., Liu, Tracy, and Ou, Li

Subjects

*LABORATORY mice, *B cell receptors, *IMMUNOGLOBULINS, *GERMINAL centers, *CIRCUMSPOROZOITE protein

Abstract

Repeat antigens, such as the Plasmodium falciparum circumsporozoite protein (PfCSP), use both sequence degeneracy and structural diversity to evade the immune response. A few PfCSP-directed antibodies have been identified that are effective at preventing malaria infection, including CIS43, but how these repeat-targeting antibodies might be improved has been unclear. Here, we engineered a humanized mouse model in which B cells expressed inferred human germline CIS43 (iGL-CIS43) B cell receptors and used both vaccination and bioinformatic analysis to obtain variant CIS43 antibodies with improved protective capacity. One such antibody, iGL-CIS43.D3, was significantly more potent than the current best-in-class PfCSP-directed antibody. We found that vaccination with a junctional epitope peptide was more effective than full-length PfCSP at recruiting iGL-CIS43 B cells to germinal centers. Structure-function analysis revealed multiple somatic hypermutations that combinatorically improved protection. This mouse model can thus be used to understand vaccine immunogens and to develop highly potent anti-malarial antibodies. [Display omitted] • Generated a knockin mouse with B cells expressing the inferred germline of CIS43 • Vaccination with junctional-epitope peptide is more effective than full-length PfCSP • Engineered a best-in-class malaria-protective antibody, iGL-CIS43.D3 • Structure and informatics analyses revealed alterations improving protective efficacy CIS43 is a malaria-protective antibody targeting a junctional epitope of the Plasmodium falciparum circumsporozoite protein. Kratochvil et al. engineer a mouse model expressing inferred germline CIS43 antibodies and use an immunofocusing strategy, in tandem with bioinformatic sieving, to generate improved CIS43 antibodies, including iGL-CIS43.D3, a best-in-class malaria-protective antibody. [ABSTRACT FROM AUTHOR]

Published

2021

12. Priority Triangular norms and their applications in Fuzzy Constraint Satisfaction Problems

Subjects

Schur-konkavnost, prioritet, fazi, fazi relacione baze podataka, fuzzy, priority, t-norme, PFCSP, fuzzy relational databases, fazi SQL, Schur-concavity, fuzzy SQL

Abstract

Doktorska disertacija pripada oblasti fazi skupova, inteligentnih sistema i baza podataka.Osnovni cilj ove teze je koriˇs´cenje konkretnih rezultate iz oblasti fazi skupovai PFCSP sistema u okviru fazi relacionih baza podataka. U skladu sa tim implementiranaje aplikacija koja ilustruje ove primene.U doktorskoj disertaciji su obrad¯ene t-norme prioriteta, jer imaju znaˇcajnu ulogu uPFCSP sistemima. T-norme prioriteta su ustvari Schur-konkavne t-norme. Originalnidoprinos autora je karakterizacija jedne klase konkavnih t-normi preko nivoskih linija(teorema 2.3).Od inteligentnih sistema prouˇcavani su PFCSP sistemi i specijalne fazi relacionebaze podataka. PFCSP (engleski Priority Fuzzy Constraint Satisfaction Problem) susistemi koji se koriste za odluˇcivanje kada ograniˇcenja mogu imati fazi vrednosti irazliˇcite prioritete. Autor je uveo novi tip PFCSP sistema koji definiˇsu stroˇziji konceptprioriteta.Svaki model zasnovan na klasiˇcnoj logici pretpostavlja dihotomiju, med¯utim u realnimsistemima ˇcesto se ne vidi granica izmed¯u dve alternative. Ukratko, fazi logikapredstavlja fleksibilan sistem koji se koristi kao semantiˇcka osnova za prirodne jezike.Preslikavanja iz jediniˇcnog kvadrata na jediniˇcni interval koja su monotona, komutativna,asocijativna i imaju jediniˇcni element 1 nazivaju se t-norme. Uopˇstenjeoperatora konjukcije u fazi logici su t-norme.Schur-konkavnost je specijalna vrsta konkavnosti. Za funkciju dve promenjivef kaˇzemo da je Schur-konkavna ako za svako x, y, u, v takvo da x + y = u + v,x ≤ u ≤ v ≤ y vaˇzi: f(u, v) ≥ f(x, y). One se primenjuju u PFCSP sistemima kaooperatori koji agregiraju lokalne mere zadovoljenja ograniˇcenja u globalnu meru.CSP (eng. Constraint satisfaction problems) sistemi koriˇs´ceni su za apstrakcijupraktiˇcnih problema. Fazifikacijom CSP sistema dobijamo FCSP (eng. Fuzzy constraint satisfaction problems) sisteme kod kojih su ograniˇcenja modelirana kao fazipodskupovi domena ili Dekartovog proizvoda nekog podskupa skupa domena. Cˇ estose deˇsava da ograniˇcenja nemaju isti prioritet, odnosno da je jedno malo ”vaˇznije oddrugog”. Zbog toga je prioritet aksiomatski uveden u FSCP sisteme i dobijeni suPFCSP sistemi.Razvojem raˇcunara sredinom devedesetih godina relacioni model postaje standardu bazama podataka. Jedan od nedostataka ovog modela bio je ˇsto nije omogu´cavaoneodred¯ene i neegzaktne vrednosti podataka. Koriˇs´cenje fazi skupova i fazi logike zaproˇsirenje relacionog modela jedan je od naˇcina za ispravljanje ovog nedostatka, ˇstorezultuje dobijanjem fazi relacionih baza podataka. Oslanjaju´ci se na PFCSP sistemeproˇsiruje se i SQL, ˇsto rezultira PFSQL-om jezikom za postavljanje upita nad fazibazom podataka kod kojih se pojavljuju uslovi sa razliˇcitim prioritetom., The scientific fields of this thesis are fuzzy sets, intelligent systems and databases.The goal of the thesis is to use results obtained in the field of fuzzy sets in PFCSPsystems and databases. According to that, a software package has been implemented.In the PhD thesis priority t-norms have been studied, since they play an importantrole in PFCSP systems. Priority t-norms are actually Schur-concave t-norms. Theoriginal contribution of the author is the characterization of a class of concave t-normsby their level lines.From the field of intelligent systems PFCSP systems have been studied. PFCSP(Priority Fuzzy Constraint Satisfaction Problem) are used for decision making whenthe constraints are fuzzy with different priorities. Author had found a new type ofPFCSP systems which define a stricter concept of priority.Each model based on classical logic imposes dichotomy. However, the differencebetween two alternatives is not always clear. Fuzzy logic represents a flexible systemused as a semantic base for natural languages.Mappings form the unit square to the unit intervals that are monotone, symmetric,associative and 1 is their unit element are called t-norms. They are a generalization ofthe conjunction operator from classical logic.Schur-concavity is a special type of concavity. If for a function the following holdsfor each x, y, u, v such that x+y = u+v, x ≤ u ≤ v ≤ y then f(u, v) ≥ f(x, y), thefunction is called Schur-concave. They are used in PFCSP systems as operators thataggregate local satisfaction degrees in order to obtain the global satisfaction degree.CSP (Constraint satisfaction problems) are used to model practical problems. Fuzzyficationof CSP leads to FCSP (Fuzzy constraint satisfaction problems) systems whichallow fuzzy values constraint satisfaction. It is common that the constraints do nothave the same priority, thus priority is axiomatically induced into FCSP resulting inPFCSP.With the development of computers in the mid nineties relational model becamethe standard in the filed of databases. One of its flaws is the lack of representation forincomplete and imprecise information. The use if fuzzy theory in order to expand therelational model is a way to correct this flaw, resulting in fuzzy relational databases.Relying of PFCSP systems SQL is also expanded resulting in PFSQL language whichallows different priorities of query conditions.

Published

2006