Immunization with SPf66 and subsequent infection with homologous and heterologous Plasmodium falciparum parasites

被引：7

作者：

Masinde, GL

Krogstad, DJ

Gordon, DM

Duffy, PE

机构：

[1] Tulane Univ, Sch Publ Hlth & Trop Med, Dept Trop Med, New Orleans, LA 70112 USA

[2] Kenya Med Res Inst, Nairobi, Kenya

[3] USA, Med Res Unit, Kisumu, Kenya

来源：

AMERICAN JOURNAL OF TROPICAL MEDICINE AND HYGIENE | 1998年 / 59卷 / 04期

关键词：

D O I：

10.4269/ajtmh.1998.59.600

中图分类号：

R1 [预防医学、卫生学];

学科分类号：

1004 ; 120402 ;

摘要：

In an area of intense transmission, a malaria vaccine could reduce infection due to the parasite types represented in the vaccine, but have no detectable effect on the overall frequency of infection if it did not protect against infection with heterologous parasites. These studies were performed to determine whether immunization with SPf66 decreased infection with homologous parasites containing the 11 amino acid peptide from merozoite surface protein-1 (MSP-1) in SPf66, or increased infection due to heterologous parasites containing heterologous (alternative) MSP-1 sequences. Based on this 11 amino acid peptide (YSLFQKEKMVL), three forward primers (S,Q,V) were designed to amplify the MSP-1 sequence present in SPf66, and 3 additional forward primers (G,H,I) to amplify the alternative MSP-1 sequence (YGLFHKEKMIL). This strategy was validated by polymerase chain reaction (PCR) amplification and dideoxy sequencing with 14 cloned laboratory isolates, which demonstrated that each primer amplified one MSP-1 sequence or the other, but not both. The technique was then used to examine filter paper blots from an SPf66 vaccine study of 69 subjects in Saradidi, Kenya. In that study, the prevalence of infection with YSLFQKEKMVL, or YGLFHKEKMIL type parasites was unaffected by immunization with SPf66 (based on PCR amplification with the S,Q,V,G, H and I primers, respectively). These results suggest that immunization with SPf66 does not produce a selective effect in vivo. They demonstrate a molecular method to test for selection in vivo as an indirect measure of vaccine efficacy.

引用

页码：600 / 605

页数：6

共 19 条

[1] RANDOMIZED TRIAL OF EFFICACY OF SPF66 VACCINE AGAINST PLASMODIUM-FALCIPARUM MALARIA IN CHILDREN IN SOUTHERN TANZANIA [J].

ALONSO, PL ;

SMITH, T ;

SCHELLENBERG, JRMA ;

MASANJA, H ;

MWANKUSYE, S ;

URASSA, H ;

DEAZEVEDO, IB ;

CHONGELA, J ;

KOBERO, S ;

MENENDEZ, C ;

HURT, N ;

THOMAS, MC ;

LYIMO, E ;

WEISS, NA ;

HAYES, R ;

KITUA, AY ;

LOPEZ, MC ;

KILAMA, WL ;

TEUSCHER, T ;

TANNER, M .

LANCET, 1994, 344 (8931) :1175-1181

[2] THE 1ST FIELD TRIALS OF THE CHEMICALLY SYNTHESIZED MALARIA VACCINE SPF66 - SAFETY, IMMUNOGENICITY AND PROTECTIVITY [J].

AMADOR, R ;

MORENO, A ;

VALERO, V ;

MURILLO, L ;

MORA, AL ;

ROJAS, M ;

ROCHA, C ;

SALCEDO, M ;

GUZMAN, F ;

ESPEJO, F ;

NUNEZ, F ;

PATARROYO, ME .

VACCINE, 1992, 10 (03) :179-184

[3] PLASMODIUM-FALCIPARUM INCIDENCE RELATIVE TO ENTOMOLOGIC INOCULATION RATES AT A SITE PROPOSED FOR TESTING MALARIA VACCINES IN WESTERN KENYA [J].

BEIER, JC ;

OSTER, CN ;

ONYANGO, FK ;

BALES, JD ;

SHERWOOD, JA ;

PERKINS, PV ;

CHUMO, DK ;

KOECH, DV ;

WHITMIRE, RE ;

ROBERTS, CR ;

DIGGS, CL ;

HOFFMAN, SL .

AMERICAN JOURNAL OF TROPICAL MEDICINE AND HYGIENE, 1994, 50 (05) :529-536

[4] EFFICACY TRIAL OF MALARIA VACCINE SPF66 IN GAMBIAN INFANTS [J].

DALESSANDRO, U ;

LEACH, A ;

DRAKELEY, CJ ;

BENNETT, S ;

OLALEYE, BO ;

FEGAN, GW ;

JAWARA, M ;

LANGEROCK, P ;

GEORGE, MO ;

TARGETT, GAT ;

GREENWOOD, BM .

LANCET, 1995, 346 (8973) :462-467

[5]

Krogstad DJ, 1996, EPIDEMIOL REV, V18, P77, DOI 10.1093/oxfordjournals.epirev.a017918

[6] ANALYSIS OF SEQUENCE DIVERSITY IN THE PLASMODIUM-FALCIPARUM MEROZOITE SURFACE PROTEIN-1 (MSP-1) [J].

MILLER, LH ;

ROBERTS, T ;

SHAHABUDDIN, M ;

MCCUTCHAN, TF .

MOLECULAR AND BIOCHEMICAL PARASITOLOGY, 1993, 59 (01) :1-14

[7] Randomised double-blind placebo-controlled trial of SPf66 malaria vaccine in children in northwestern Thailand [J].

Nosten, F ;

Luxemburger, C ;

Kyle, DE ;

Ballou, WR ;

Wittes, J ;

Wah, E ;

Chongsuphajaisiddhi, T ;

Gordon, DM ;

White, NJ ;

Sadoff, JC ;

Heppner, DG ;

Bathe, K ;

Blood, J ;

Brockman, A ;

Cobley, UT ;

Hacking, D ;

Hogg, D ;

U, KH ;

Maelankiri, L ;

Chuanak, N ;

Permpanich, B ;

Price, R ;

Raimond, D ;

Schabenberger, O ;

Singharaj, P ;

Singhasivanon, P ;

Slight, T ;

Tulayon, S ;

Tway, KL ;

Ynint, T ;

VincentiDelmas, M ;

deVries, A ;

Webster, HK .

LANCET, 1996, 348 (9029) :701-707

[8] A POPULATION-BASED CLINICAL-TRIAL WITH THE SPF66 SYNTHETIC PLASMODIUM-FALCIPARUM MALARIA VACCINE IN VENEZUELA [J].

NOYA, O ;

BERTI, YG ;

DENOYA, BA ;

BORGES, R ;

ZERPA, N ;

URBAEZ, JD ;

MADONNA, A ;

GARRIDO, E ;

JIMENEZ, MA ;

BORGES, RE ;

GARCIA, P ;

REYES, I ;

PRIETO, W ;

COLMENARES, C ;

PABON, R ;

BARRAEZ, T ;

DECACERES, LG ;

GODOY, N ;

SIFONTES, R .

JOURNAL OF INFECTIOUS DISEASES, 1994, 170 (02) :396-402

[9] MALARIA VACCINES - MULTIPLE TARGETS [J].

NUSSENZWEIG, RS ;

LONG, CA .

SCIENCE, 1994, 265 (5177) :1381-1383

[10] INDUCTION OF PROTECTIVE IMMUNITY AGAINST EXPERIMENTAL-INFECTION WITH MALARIA USING SYNTHETIC PEPTIDES [J].

PATARROYO, ME ;

ROMERO, P ;

TORRES, ML ;

CLAVIJO, P ;

MORENO, A ;

MARTINEZ, A ;

RODRIGUEZ, R ;

GUZMAN, F ;

CABEZAS, E .

NATURE, 1987, 328 (6131) :629-632

← 1 2 →