Potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients

Potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients

Abstract Neoplasm development in Multiple Sclerosis (MS) patients treated with disease-modifying therapies (DMTs) has been widely discussed. The aim of this work is to determine neoplasm frequency, relationship with the prescription pattern of DMTs, and influence of the patients’ baseline characteri...

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Main Authors: Rosalía Gil-Bernal, Juan Luis González-Caballero, Raúl Espinosa-Rosso, Carmen Gómez-Gómez
Format: Article
Language:English
Published: Nature Publishing Group 2021-06-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-021-91912-x
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spelling doaj-9e0434f4136d47b6b5db10f717e474812021-06-20T11:34:37ZengNature Publishing GroupScientific Reports2045-23222021-06-011111910.1038/s41598-021-91912-xPotential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatientsRosalía Gil-Bernal0Juan Luis González-Caballero1Raúl Espinosa-Rosso2Carmen Gómez-Gómez3Department of Biochemistry, Faculty of Medicine, University of CadizDepartment of Statistics and Operations Research, Faculty of Medicine, University of CadizDepartment of Neurology, Hospital Universitario Puerta del Mar (HUPM)Department of Biochemistry, Faculty of Medicine, University of CadizAbstract Neoplasm development in Multiple Sclerosis (MS) patients treated with disease-modifying therapies (DMTs) has been widely discussed. The aim of this work is to determine neoplasm frequency, relationship with the prescription pattern of DMTs, and influence of the patients’ baseline characteristics. Data from 250 MS outpatients were collected during the period 1981–2019 from the medical records of the Neurology Service of the HUPM (Hospital Universitario Puerta del Mar)—in Southern Spain—and analysed using Cox models. Neoplasm prevalence was 24%, mainly located on the skin, with cancer prevalence as expected for MS (6.8%). Latency period from MS onset to neoplasm diagnosis was 10.4 ± 6.9 years (median 9.30 [0.9–30.5]). During the observation period β-IFN (70.4% of patients), glatiramer acetate (30.4%), natalizumab (16.8%), fingolimod (24.8%), dimethyl fumarate (24.0%), alemtuzumab (6.0%), and teriflunomide (4.8%) were administered as monotherapy. Change of pattern in step therapy was significantly different in cancer patients vs unaffected individuals (p = 0.011) (29.4% did not receive DMTs [p = 0.000]). Extended Cox model: Smoking (HR = 3.938, CI 95% 1.392–11.140, p = 0.010), being female (HR = 2.006, 1.070–3.760, p = 0.030), and age at MS diagnosis (AGE-DG) (HR = 1.036, 1.012–1.061, p = 0.004) were risk factors for neoplasm development. Secondary progressive MS (SPMS) phenotype (HR = 0.179, 0.042–0.764, p = 0.020) and treatment-time with IFN (HR = 0.923, 0.873–0.977, p = 0.006) or DMF (HR = 0.725, 0.507–1.036, p = 0.077) were protective factors. Tobacco and IFN lost their negative/positive influence as survival time increased. Cox PH model: Tobacco/AGE-DG interaction was a risk factor for cancer (HR = 1.099, 1.001–1.208, p = 0.049), followed by FLM treatment-time (HR = 1.219, 0.979–1.517). In conclusion, smoking, female sex, and AGE-DG were risk factors, and SPMS and IFN treatment-time were protective factors for neoplasm development; smoking/AGE-DG interaction was the main cancer risk factor.https://doi.org/10.1038/s41598-021-91912-x
collection DOAJ
language English
format Article
sources DOAJ
author Rosalía Gil-Bernal
Juan Luis González-Caballero
Raúl Espinosa-Rosso
Carmen Gómez-Gómez
spellingShingle Rosalía Gil-Bernal
Juan Luis González-Caballero
Raúl Espinosa-Rosso
Carmen Gómez-Gómez
Potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients
Scientific Reports
author_facet Rosalía Gil-Bernal
Juan Luis González-Caballero
Raúl Espinosa-Rosso
Carmen Gómez-Gómez
author_sort Rosalía Gil-Bernal
title Potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients
title_short Potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients
title_full Potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients
title_fullStr Potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients
title_full_unstemmed Potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients
title_sort potential risk of disease modifying therapies on neoplasm development and coadjutant factors in multiple sclerosis outpatients
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-06-01
description Abstract Neoplasm development in Multiple Sclerosis (MS) patients treated with disease-modifying therapies (DMTs) has been widely discussed. The aim of this work is to determine neoplasm frequency, relationship with the prescription pattern of DMTs, and influence of the patients’ baseline characteristics. Data from 250 MS outpatients were collected during the period 1981–2019 from the medical records of the Neurology Service of the HUPM (Hospital Universitario Puerta del Mar)—in Southern Spain—and analysed using Cox models. Neoplasm prevalence was 24%, mainly located on the skin, with cancer prevalence as expected for MS (6.8%). Latency period from MS onset to neoplasm diagnosis was 10.4 ± 6.9 years (median 9.30 [0.9–30.5]). During the observation period β-IFN (70.4% of patients), glatiramer acetate (30.4%), natalizumab (16.8%), fingolimod (24.8%), dimethyl fumarate (24.0%), alemtuzumab (6.0%), and teriflunomide (4.8%) were administered as monotherapy. Change of pattern in step therapy was significantly different in cancer patients vs unaffected individuals (p = 0.011) (29.4% did not receive DMTs [p = 0.000]). Extended Cox model: Smoking (HR = 3.938, CI 95% 1.392–11.140, p = 0.010), being female (HR = 2.006, 1.070–3.760, p = 0.030), and age at MS diagnosis (AGE-DG) (HR = 1.036, 1.012–1.061, p = 0.004) were risk factors for neoplasm development. Secondary progressive MS (SPMS) phenotype (HR = 0.179, 0.042–0.764, p = 0.020) and treatment-time with IFN (HR = 0.923, 0.873–0.977, p = 0.006) or DMF (HR = 0.725, 0.507–1.036, p = 0.077) were protective factors. Tobacco and IFN lost their negative/positive influence as survival time increased. Cox PH model: Tobacco/AGE-DG interaction was a risk factor for cancer (HR = 1.099, 1.001–1.208, p = 0.049), followed by FLM treatment-time (HR = 1.219, 0.979–1.517). In conclusion, smoking, female sex, and AGE-DG were risk factors, and SPMS and IFN treatment-time were protective factors for neoplasm development; smoking/AGE-DG interaction was the main cancer risk factor.
url https://doi.org/10.1038/s41598-021-91912-x
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