Soluble programmed death‐1 (sPD‐1) as predictor of early surgical outcomes of paediatric cystic echinococcosis

Aims Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death‐1 (sPD‐1), sPD‐1 ligand (sPD‐L1) and anti‐recP29 antibody concentrations, as predictors of early surgical treatment outcomes in young CE‐affected pat...

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Published inParasite immunology Vol. 43; no. 3; pp. e12809 - n/a
Main Authors Ben Salah, Eya, Sakly, Wahiba, Barrera, Coralie, Mosbahi, Sana, Bellanger, Anne‐Pauline, Farhani, Rabeb, Ksia, Amine, Gottstein, Bruno, Nouri, Abdellatif, Babba, Hamouda, Millon, Laurence
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Published England Wiley Subscription Services, Inc 01.03.2021
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Abstract Aims Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death‐1 (sPD‐1), sPD‐1 ligand (sPD‐L1) and anti‐recP29 antibody concentrations, as predictors of early surgical treatment outcomes in young CE‐affected patients. Methods and results This prospective study included 59 Tunisian children (177 plasmas), where CE was surgically treated and monitored for 3 post‐operative years. Based on CE post‐surgical development, patients were clustered into a ‘No relapsed’ CE (NRCE; n = 39) and a ‘Relapsed’ CE (RCE; n = 20) group. Plasma levels of sPD‐1, sPD‐L1 and anti‐recP29 IgG were measured using ELISA. In the NRCE group, sPD‐1, sPD‐L1 and anti‐recP29 IgG concentrations were significantly lower at D365 than at D30. By contrast, in the RCE group, no significant difference was observed between D0, D30 and D365. When considering individual variations, the probability to be ‘relapse‐free’ was 67% and 73% when anti‐recP29 IgG and sPD‐L1 level, respectively, decreased between D30 and D365. The probability to be ‘relapse‐free’ was 86% when the sPD‐1 level decreased between D30 and D365 (P = .003; chi‐square test). Conclusion sPD‐1 may be a useful biomaker for the early evaluation of surgical procedure efficacy in paediatric CE cases. Ben Salah et al. assess the value of two costimulatory molecules; soluble programmed death‐1 (sPD‐1), sPD‐1 ligand (sPD‐L1) as well anti‐recP29 antibodies concentrations as early predictors of operative procedure efficacy in paediatric cystic echinococcosis. Our findings show that sPD‐1 may be a promising biomaker for the early evaluation of surgical treatment outcomes in young CE cases..
AbstractList AimsFollowing treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death‐1 (sPD‐1), sPD‐1 ligand (sPD‐L1) and anti‐recP29 antibody concentrations, as predictors of early surgical treatment outcomes in young CE‐affected patients.Methods and resultsThis prospective study included 59 Tunisian children (177 plasmas), where CE was surgically treated and monitored for 3 post‐operative years. Based on CE post‐surgical development, patients were clustered into a ‘No relapsed’ CE (NRCE; n = 39) and a ‘Relapsed’ CE (RCE; n = 20) group. Plasma levels of sPD‐1, sPD‐L1 and anti‐recP29 IgG were measured using ELISA. In the NRCE group, sPD‐1, sPD‐L1 and anti‐recP29 IgG concentrations were significantly lower at D365 than at D30. By contrast, in the RCE group, no significant difference was observed between D0, D30 and D365. When considering individual variations, the probability to be ‘relapse‐free’ was 67% and 73% when anti‐recP29 IgG and sPD‐L1 level, respectively, decreased between D30 and D365. The probability to be ‘relapse‐free’ was 86% when the sPD‐1 level decreased between D30 and D365 (P = .003; chi‐square test).ConclusionsPD‐1 may be a useful biomaker for the early evaluation of surgical procedure efficacy in paediatric CE cases.
Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death-1 (sPD-1), sPD-1 ligand (sPD-L1) and anti-recP29 antibody concentrations, as predictors of early surgical treatment outcomes in young CE-affected patients.
Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death-1 (sPD-1), sPD-1 ligand (sPD-L1) and anti-recP29 antibody concentrations, as predictors of early surgical treatment outcomes in young CE-affected patients. This prospective study included 59 Tunisian children (177 plasmas), where CE was surgically treated and monitored for 3 post-operative years. Based on CE post-surgical development, patients were clustered into a 'No relapsed' CE (NRCE; n = 39) and a 'Relapsed' CE (RCE; n = 20) group. Plasma levels of sPD-1, sPD-L1 and anti-recP29 IgG were measured using ELISA. In the NRCE group, sPD-1, sPD-L1 and anti-recP29 IgG concentrations were significantly lower at D365 than at D30. By contrast, in the RCE group, no significant difference was observed between D0, D30 and D365. When considering individual variations, the probability to be 'relapse-free' was 67% and 73% when anti-recP29 IgG and sPD-L1 level, respectively, decreased between D30 and D365. The probability to be 'relapse-free' was 86% when the sPD-1 level decreased between D30 and D365 (P = .003; chi-square test). sPD-1 may be a useful biomaker for the early evaluation of surgical procedure efficacy in paediatric CE cases.
Aims Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death‐1 (sPD‐1), sPD‐1 ligand (sPD‐L1) and anti‐recP29 antibody concentrations, as predictors of early surgical treatment outcomes in young CE‐affected patients. Methods and results This prospective study included 59 Tunisian children (177 plasmas), where CE was surgically treated and monitored for 3 post‐operative years. Based on CE post‐surgical development, patients were clustered into a ‘No relapsed’ CE (NRCE; n = 39) and a ‘Relapsed’ CE (RCE; n = 20) group. Plasma levels of sPD‐1, sPD‐L1 and anti‐recP29 IgG were measured using ELISA. In the NRCE group, sPD‐1, sPD‐L1 and anti‐recP29 IgG concentrations were significantly lower at D365 than at D30. By contrast, in the RCE group, no significant difference was observed between D0, D30 and D365. When considering individual variations, the probability to be ‘relapse‐free’ was 67% and 73% when anti‐recP29 IgG and sPD‐L1 level, respectively, decreased between D30 and D365. The probability to be ‘relapse‐free’ was 86% when the sPD‐1 level decreased between D30 and D365 (P = .003; chi‐square test). Conclusion sPD‐1 may be a useful biomaker for the early evaluation of surgical procedure efficacy in paediatric CE cases. Ben Salah et al. assess the value of two costimulatory molecules; soluble programmed death‐1 (sPD‐1), sPD‐1 ligand (sPD‐L1) as well anti‐recP29 antibodies concentrations as early predictors of operative procedure efficacy in paediatric cystic echinococcosis. Our findings show that sPD‐1 may be a promising biomaker for the early evaluation of surgical treatment outcomes in young CE cases..
Abstract Aims Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death‐1 (sPD‐1), sPD‐1 ligand (sPD‐L1) and anti‐recP29 antibody concentrations, as predictors of early surgical treatment outcomes in young CE‐affected patients. Methods and results This prospective study included 59 Tunisian children (177 plasmas), where CE was surgically treated and monitored for 3 post‐operative years. Based on CE post‐surgical development, patients were clustered into a ‘No relapsed’ CE (NRCE; n = 39) and a ‘Relapsed’ CE (RCE; n = 20) group. Plasma levels of sPD‐1, sPD‐L1 and anti‐recP29 IgG were measured using ELISA. In the NRCE group, sPD‐1, sPD‐L1 and anti‐recP29 IgG concentrations were significantly lower at D365 than at D30. By contrast, in the RCE group, no significant difference was observed between D0, D30 and D365. When considering individual variations, the probability to be ‘relapse‐free’ was 67% and 73% when anti‐recP29 IgG and sPD‐L1 level, respectively, decreased between D30 and D365. The probability to be ‘relapse‐free’ was 86% when the sPD‐1 level decreased between D30 and D365 ( P  = .003; chi‐square test). Conclusion sPD‐1 may be a useful biomaker for the early evaluation of surgical procedure efficacy in paediatric CE cases.
Author Barrera, Coralie
Gottstein, Bruno
Farhani, Rabeb
Sakly, Wahiba
Ksia, Amine
Nouri, Abdellatif
Mosbahi, Sana
Babba, Hamouda
Millon, Laurence
Ben Salah, Eya
Bellanger, Anne‐Pauline
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CitedBy_id crossref_primary_10_3390_pathogens13060477
crossref_primary_10_3390_pathogens12091116
crossref_primary_10_1016_j_jinf_2021_09_023
crossref_primary_10_1186_s13071_021_04679_5
crossref_primary_10_1097_QCO_0000000000000941
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Keywords follow-up
recP29
sPD-1
cystic echinococcosis
children
post-surgical outcome
sPD-L1
Language English
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Snippet Aims Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death‐1...
Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death-1 (sPD-1),...
Abstract Aims Following treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed...
AimsFollowing treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death‐1...
AIMSFollowing treatment, cystic echinococcosis (CE) exhibits a relatively high relapse rate. Here, we evaluated the value of soluble programmed death-1...
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StartPage e12809
SubjectTerms Adolescent
B7-H1 Antigen
Biomarkers
Child
Child, Preschool
children
cystic echinococcosis
Echinococcosis
Ecology, environment
Enzyme-Linked Immunosorbent Assay
Female
follow‐up
Health
Humans
Immunoglobulin G
Life Sciences
Male
PD-1 protein
Pediatrics
Plasma levels
post‐surgical outcome
Prospective Studies
recP29
Secondary Prevention
sPD‐1
sPD‐L1
Treatment Outcome
Title Soluble programmed death‐1 (sPD‐1) as predictor of early surgical outcomes of paediatric cystic echinococcosis
URI https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fpim.12809
https://www.ncbi.nlm.nih.gov/pubmed/33207012
https://www.proquest.com/docview/2491605444
https://search.proquest.com/docview/2462411274
https://hal.science/hal-03316048
Volume 43
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