Trypanosoma cruzi loop-mediated isothermal amplification (Trypanosoma cruzi Loopamp) kit for detection of congenital, acute and Chagas disease reactivation

Besuschio, S; Picado, Albert; Muñoz-Calderón, Arturo; Wehrendt, Diana Patricia; Fernández, Marisa; Benatar, Alejandro Francisco; Díaz-Bello, Zoraida; Irurtia, Cecilia; Cruz, Israel; Ndung’u, Joseph Mathu; Cafferata, María Luisa; Montenegro, Graciela; Estani, Sérgio Sosa; Lucero, Raúl Horacio; Noya, Belkisyolé Alarcón de; Longhi, Silvia Andrea; Schijman, Alejandro G.

doi:10.1371/journal.pntd.0008402

Cited by 26 publications

(35 citation statements)

References 42 publications

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“…In this work, monitoring for CDR was made in 48.1% of patients with co-infection by parasitological enrichment methods, and more rarely, by PCR. Quantitative PCR represents a safety test to monitor parasitemia in immunocompromised hosts when able to differentiate between higher parasitemia in CDR and lower parasitemia in non-reactivation episodes of the co-infection [ 22 , 38 , 42 , 43 ]. Therefore, its implementation is essential for CDR detection as rapidly as possible in order to adapt immunosuppressive treatment and to start the anti-parasitic treatment.…”

Section: Discussionmentioning

confidence: 99%

Clinical profile and mortality in patients with T. cruzi/HIV co-infection from the multicenter data base of the “Network for healthcare and study of Trypanosoma cruzi/HIV co-infection and other immunosuppression conditions”

et al. 2021

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Objective Chagas disease (CD) globalization facilitated the co-infection with Human Immunodeficiency Virus (HIV) in endemic and non-endemic areas. Considering the underestimation of Trypanosoma cruzi (T. cruzi)-HIV co-infection and the risk of life-threatening Chagas Disease Reactivation (CDR), this study aimed to analyze the major co-infection clinical characteristics and its mortality rates. Methods This is a cross-sectional retrospective multicenter study of patients with CD confirmed by two serological or one parasitological tests, and HIV infection confirmed by immunoblot. CDR was diagnosed by direct microscopy with detection of trypomastigote forms in the blood or other biological fluids and/or amastigote forms in inflammatory lesions. Results Out of 241 patients with co-infection, 86.7% were from Brazil, 47.5% had <200 CD4+ T cells/μL and median viral load was 17,000 copies/μL. Sixty CDR cases were observed. Death was more frequent in patients with reactivation and was mainly caused by CDR. Other causes of death unrelated to CDR were the manifestation of opportunistic infections in those with Acquired Immunodeficiency Syndrome. The time between the co-infection diagnosis to death was shorter in patients with CDR. Lower CD4+ cells count at co-infection diagnosis was independently associated with reactivation. Similarly, lower CD4+ cells numbers at co-infection diagnosis and male sex were associated with higher lethality in CDR. Additionally, CD4+ cells were lower in meningoencephalitis than in myocarditis and milder forms. Conclusion This study showed major features on T. cruzi-HIV co-infection and highlighted the prognostic role of CD4+ cells for reactivation and mortality. Since lethality was high in meningoencephalitis and all untreated patients died shortly after the diagnosis, early diagnosis, immediate antiparasitic treatment, patient follow-up and epidemiological surveillance are essentials in T. cruzi/HIV co-infection and CDR managements.

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Section: Discussionmentioning

confidence: 99%

Clinical profile and mortality in patients with T. cruzi/HIV co-infection from the multicenter data base of the “Network for healthcare and study of Trypanosoma cruzi/HIV co-infection and other immunosuppression conditions”

et al. 2021

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“…However, Besuschio et al tested a LAMP prototype kit, so far not commercially available, on a series of archival DNA samples from acutely infected patients and found sensitivity and specificity values of 93% and 100%, respectively [ 15 , 16 ]. All the samples they obtained from CCD-infected patients (average age 108 days old) yielded positive LAMP results and the parasitic loads found were between 5.27 and 3063.47 par.…”

Section: Discussionmentioning

confidence: 99%

“…All the samples they obtained from CCD-infected patients (average age 108 days old) yielded positive LAMP results and the parasitic loads found were between 5.27 and 3063.47 par. eq/mL [ 15 , 16 ]. Because the performance of the molecular tests will critically depend on the copy number of the target sequences, probably, increased sensitivity was possible because this prototype kit is targeted to satellite DNA sequences (a higher copy number than the 18S rRNA genes).…”

Section: Discussionmentioning

confidence: 99%

“…for T. cruzi detection [14][15][16]. Before implementation into routine clinical practice and incorporation into guidelines, every new diagnostic assay should go through a lengthy validation process.…”

Section: Key Pointsmentioning

confidence: 99%

“…Over 20 years, the PCR technique has been presented as a promising tool for sensitive and specific detection of T. cruzi parasites [ 11 – 13 ]. Furthermore, isothermal DNA amplification (LAMP), which requires less infrastructure, has been reported as a possible molecular diagnostic tool for T. cruzi detection [ 14 – 16 ]. Before implementation into routine clinical practice and incorporation into guidelines, every new diagnostic assay should go through a lengthy validation process.…”

Section: Introductionmentioning

confidence: 99%

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Diagnostic Accuracy of Two Molecular Tools for Diagnosis of Congenital Chagas Disease

et al. 2021

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Background and Objective The real prevalence of congenital Chagas disease is undefined because of difficulties in the detection of Trypanosoma cruzi by microscopic examination. The aim of this study was to determine the diagnostic accuracy of two molecular diagnostic tools, qPCR and LAMP, in the diagnosis of congenital Chagas disease in a clinical setting. Methods To this end, we conducted a prospective cohort study in a tertiary care center, of infants under 9 months of age, born in Buenos Aires to women with Chagas disease. Blood samples were collected for microscopic examination and molecular diagnosis at baseline. If negative, infants were followed up until 9 months of age to determine a final diagnosis by serology. In-house qPCR and LAMP previously validated were challenged as index tests. Results A total of 154 participants were potentially eligible, 120 of whom were enrolled. Finally, 102 (66.2%) of them fulfilled the follow-up. The diagnosis of congenital Chagas disease was confirmed in 13 infants and excluded in 89. Both the sensitivity and specificity of the qPCR were 100.0% (95% confidence interval 75.3–100.0 and 95% confidence interval 95.9–100.0, respectively), whereas the sensitivity and specificity of LAMP were 69.2% (95% confidence interval 38.6–90.9) and 100% (95% confidence interval 95.9–100.0), respectively. Conclusions The qPCR agreed with the current diagnostic algorithm, and was a reliable and sensitive tool to detect congenital Chagas disease earlier, providing an appropriate and timely identification of infected infants requiring treatment. LAMP was able to detect congenital Chagas disease in infected infants by naked-eye visualization in accordance with a microscopic examination. The advantages of molecular diagnostic tools should be taken into account by the health system to improve congenital Chagas disease diagnosis.

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Liquid Biopsy for Promising Non-invasive Diagnostic Biomarkers in Parasitic Infections

Öztürk

Caner

2021

Acta Parasit.

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Trypanosoma cruzi loop-mediated isothermal amplification (Trypanosoma cruzi Loopamp) kit for detection of congenital, acute and Chagas disease reactivation

Cited by 26 publications

References 42 publications

Clinical profile and mortality in patients with T. cruzi/HIV co-infection from the multicenter data base of the “Network for healthcare and study of Trypanosoma cruzi/HIV co-infection and other immunosuppression conditions”

Clinical profile and mortality in patients with T. cruzi/HIV co-infection from the multicenter data base of the “Network for healthcare and study of Trypanosoma cruzi/HIV co-infection and other immunosuppression conditions”

Diagnostic Accuracy of Two Molecular Tools for Diagnosis of Congenital Chagas Disease

Liquid Biopsy for Promising Non-invasive Diagnostic Biomarkers in Parasitic Infections

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