Literature DB >> 18214203

Chloroquine-resistant Plasmodium vivax, Brazilian Amazon.

Franklin Simoes de Santana Filho, Ana Ruth de Lima Arcanjo, Yonne Melo Chehuan, Monica Regina Costa, Flor Ernestina Martinez-Espinosa, Jose Luis Vieira, Maria das Graças Vale Barbosa, Wilson Duarte Alecrim, Maria das Graças Costa Alecrim.   

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Year:  2007        PMID: 18214203      PMCID: PMC2878224          DOI: 10.3201/eid1307.061386

Source DB:  PubMed          Journal:  Emerg Infect Dis        ISSN: 1080-6040            Impact factor:   6.883


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To the Editor: Plasmodium vivax is the protozoan that causes the second most common form of malaria. Some resistant strains to chloroquine (CQ) occur in a few places in Asia and the Indo-Pacific Region (–). Although resistance of P. vivax to CQ has already been described in South America (–), there are limited data regarding this issue. CQ plus primaquine is the standard treatment for vivax malaria worldwide. Presently, this drug regimen exhibits satisfactory efficacy in the Brazilian Amazon. However, in recent years several treatment failures presumably related to CQ resistance, have been reported in the city of Manaus (Amazonas) where vivax malaria predominates (). This observation warrants local attention despite these cases having no confirmation of CQ blood levels on the basis of the appearance of asexual parasites against CQ plus desethylchloroquine levels exceeding the minimally effective plasma concentration proposed for sensitive parasite strains (>10 ng/mL) (), according to Pan American Health Organization recommendations (). From September 2004 to February 2005, a 28-day in vivo test was conducted at the Foundation for Tropical Medicine of Amazonas (FMTAM) in Manaus, Brazil, to assess the efficacy of standard supervised CQ therapy. The test involved 166 volunteers with uncomplicated vivax malaria. Each volunteer was administered uncoated, scored, 150-mg CQ tablets (10 + 7.5 + 7.5 mg/kg at 24-hour intervals) (). Primaquine was withheld until day 28 (dose regimen of 30 mg/day for 7 days). Among the 109 volunteers who completed the in vivo test, 19 had positive blood smears within the 28-day follow-up (1 on day 14, 3 on day 21, and 15 on day 28). All were required to undergo alternative therapy (mefloquine). Adequate CQ absorption was confirmed in these cases on day 2 with a mean ± SD CQ plasma concentration of 785.4 ± 800.1 ng/mL) () Suspected therapeutic failure (P. vivax CQ resistance) was confirmed in 11 (10.1%) of 109 persons with a mean isolated choloroquine plasma concentration >10 ng/mL (356.6 ± 296.1 ng/mL) (). Desethylchloroquine levels in plasma were not measured. Previously, a CQ efficacy study demonstrated that 4.4% of those tested had CQ-resistant P. vivax (). In comparison, the proportion of failures (10.1%) in the current study seems to be relevant; even though most of the P. vivax infections (98, 89.9%) were successfully evaluated and adequate clinical and parasitologic responses were obtained. Currently, the FMTAM Manaus Outpatient Clinic is detecting patients from different areas of the city who show parasitologic recurrences after correct treatment within 28 days of the routine clinical follow-up. This observation is an indirect indicator of the possible regional spread of P. vivax CQ-resistant strains (unpub. data). We believe our findings are important and merit the attention of local public health authorities. Considering the possibility of emerging underestimated P. vivax CQ resistance in Manaus, we feel it is essential to quickly clarify whether such documented resistance can copromote vivax malaria outbreaks in malaria-endemic areas within the Amazon.
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1.  Plasmodium vivax malaria in Southeast Iran in 1999-2001: establishing the response to chloroquine in vitro and in vivo.

Authors:  Y Hamedi; M Nateghpour; P Tan-ariya; M Tiensuwan; U Silachamroon; S Looareesuwan
Journal:  Southeast Asian J Trop Med Public Health       Date:  2002-09       Impact factor: 0.267

2.  Failure of combined chloroquine and high-dose primaquine therapy for Plasmodium vivax malaria acquired in Guyana, South America.

Authors:  E J Phillips; J S Keystone; K C Kain
Journal:  Clin Infect Dis       Date:  1996-11       Impact factor: 9.079

Review 3.  Diagnosis of resistance to chloroquine by Plasmodium vivax: timing of recurrence and whole blood chloroquine levels.

Authors:  J K Baird; B Leksana; S Masbar; D J Fryauff; M A Sutanihardja; F S Wignall; S L Hoffman
Journal:  Am J Trop Med Hyg       Date:  1997-06       Impact factor: 2.345

4.  In vivo resistance to chloroquine by Plasmodium vivax and Plasmodium falciparum at Nabire, Irian Jaya, Indonesia.

Authors:  J K Baird; I Wiady; D J Fryauff; M A Sutanihardja; B Leksana; H Widjaya; B Subianto
Journal:  Am J Trop Med Hyg       Date:  1997-06       Impact factor: 2.345

5.  HPLC analysis of anti-malaria agent, chloroquine in blood and tissue from forensic autopsy cases in Tanzania.

Authors:  Kosei Yonemitsu; Ako Koreeda; Kazuhiko Kibayashi; Paul Ng'walali; Martin Mbonde; James Kitinya; Shigeyuki Tsunenari
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6.  Sensitivity of Plasmodium vivax to chloroquine in Sa Kaeo Province, Thailand.

Authors:  K Congpuong; K Na-Bangchang; K Thimasarn; U Tasanor; W H Wernsdorfer
Journal:  Acta Trop       Date:  2002-08       Impact factor: 3.112

7.  Development of resistance to chloroquine by Plasmodium vivax in Myanmar.

Authors: 
Journal:  Trans R Soc Trop Med Hyg       Date:  1995 May-Jun       Impact factor: 2.184

8.  Chloroquine-resistant Plasmodium vivax malaria in Peru.

Authors:  Trenton K Ruebush; Jorge Zegarra; Javier Cairo; Ellen M Andersen; Michael Green; Dylan R Pillai; Wilmer Marquiño; María Huilca; Ernesto Arévalo; Coralith Garcia; Lely Solary; Kevin C Kain
Journal:  Am J Trop Med Hyg       Date:  2003-11       Impact factor: 2.345

  8 in total
  87 in total

1.  Next-Generation Sequencing of Plasmodium vivax Patient Samples Shows Evidence of Direct Evolution in Drug-Resistance Genes.

Authors:  Erika L Flannery; Tina Wang; Ali Akbari; Victoria C Corey; Felicia Gunawan; A Taylor Bright; Matthew Abraham; Juan F Sanchez; Meddly L Santolalla; G Christian Baldeviano; Kimberly A Edgel; Luis A Rosales; Andrés G Lescano; Vineet Bafna; Joseph M Vinetz; Elizabeth A Winzeler
Journal:  ACS Infect Dis       Date:  2015-08-03       Impact factor: 5.084

2.  Whole-genome sequencing and microarray analysis of ex vivo Plasmodium vivax reveal selective pressure on putative drug resistance genes.

Authors:  Neekesh V Dharia; A Taylor Bright; Scott J Westenberger; S Whitney Barnes; Serge Batalov; Kelli Kuhen; Rachel Borboa; Glenn C Federe; Colleen M McClean; Joseph M Vinetz; Victor Neyra; Alejandro Llanos-Cuentas; John W Barnwell; John R Walker; Elizabeth A Winzeler
Journal:  Proc Natl Acad Sci U S A       Date:  2010-10-29       Impact factor: 11.205

3.  In vitro anti-malarial drug susceptibility of temperate Plasmodium vivax from central China.

Authors:  Feng Lu; Qi Gao; Kesinee Chotivanich; Hui Xia; Jun Cao; Rachanee Udomsangpetch; Liwang Cui; Jetsumon Sattabongkot
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Review 7.  Resistance to therapies for infection by Plasmodium vivax.

Authors:  J Kevin Baird
Journal:  Clin Microbiol Rev       Date:  2009-07       Impact factor: 26.132

8.  Long-term humoral and cellular immune responses elicited by a heterologous Plasmodium vivax apical membrane antigen 1 protein prime/adenovirus boost immunization protocol.

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Review 9.  Application of pharmacogenomics to malaria: a holistic approach for successful chemotherapy.

Authors:  Rajeev K Mehlotra; Cara N Henry-Halldin; Peter A Zimmerman
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10.  Increased expression levels of the pvcrt-o and pvmdr1 genes in a patient with severe Plasmodium vivax malaria.

Authors:  Carmen Fernández-Becerra; Maria Jesús Pinazo; Ana González; Pedro L Alonso; Hernando A del Portillo; Joaquim Gascón
Journal:  Malar J       Date:  2009-04-02       Impact factor: 2.979

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