Literature DB >> 33637399

Adverse effects of polychemotherapy for leprosy in 13 years of follow-up at a university hospital.

Violeta Duarte Tortelly1, Egon Luiz Daxbacher2, Arles Martins Brotas3, Sueli Carneiro4.   

Abstract

Leprosy is one of the neglected diseases in the world and Brazil is the second country with more cases. A retrospective study was conducted based on the medical records of 196 leprosy patients diagnosed during the course of 13 years at a university hospital. The aim was to describe the adverse effects of polychemotherapy, as well the most prevalent and most vulnerable populations. In the study, dapsone was the most implicated drug, especially in women, and the risk increased with age. The authors conclude that with this patient profile, greater vigilance should be taken regarding possible adverse effects, especially anemia.
Copyright © 2021 Sociedade Brasileira de Dermatologia. Published by Elsevier España, S.L.U. All rights reserved.

Entities:  

Keywords:  Clofazimine; Dapsone; Leprosy; Rifampicin

Mesh:

Substances:

Year:  2021        PMID: 33637399      PMCID: PMC8007483          DOI: 10.1016/j.abd.2020.07.005

Source DB:  PubMed          Journal:  An Bras Dermatol        ISSN: 0365-0596            Impact factor:   1.896


Introduction

The multidrug therapy (MDT) recommended by the World Health Organization (WHO) has dramatically changed the natural history of leprosy. It reduced the prevalence and development of antimicrobial resistance. A cohort of 371 leprosy patients was followed-up for 13 years to identify the sociodemographic profile and the most frequent adverse effects of MDT.

Methods

In a retrospective study from 2002 to 2014, 371 leprosy patients were evaluated and the socio-demographic profile and adverse effects (AE) of the standard MDT were evaluated. Paucibacillary (PB) and multibacillary (MB) patients who underwent less than four and nine supervised doses, respectively, were excluded; 196 patients remained.

Results

Of the 196 patients, 97 were males and 99 females; 41.32% were treated with MDT-PB, 53.05% with MDT-MB, and 5.61% with an alternative regimen (Table 1). A total of 61 adverse effects were reported in 56 patients, of whom 64.28% (36) were women. Three patients were under 15 years of age; 12 were over 70 years; and 41 (73.21%), between 16 and 69 years. Hemolytic anemia was the most frequent adverse reaction (73.20%), whether acute (30.35%) or chronic (42.85%); 83.3% of these cases were observed in women, mainly aged 45 years or over (63.3%). The chance of a patient with anemia being female was 2.14 times greater (OR = 2.14; 95% CI: 1.14–4.12). Sulfonic syndrome occurred in two patients, while methemoglobinemia was observed in one (Table 2). Gastrointestinal alterations such as anorexia, nausea, vomiting, diarrhea, or epigastric pain were observed in nearly one-fifth of the patients, mostly (72.2%) due to DDS. Two patients presented photosensitivity. The chance of an individual having an AE increased with each year of age (OR = 1.02; 95% CI 1.00–1.04). Nonetheless, no association was observed between type of AE and age.
Table 1

Characteristics of the 196 leprosy patients followed-up at the hospital.

CharacteristicsNumberPercentage (%)
Gender
Male9749.0
Female9951.0
Ethnicity
White8442.9
Black4221.4
Asian10.5
Mixed-race6432.7
Native Brazilian00
Unknown52.5
Age (years)
11 – 202418.05
21 – 303324.81
31 – 403425.57
41 – 50139.77
51 – 60118.27
61 – 7053.76
> 70139.77
Clinical presentation
Undetermined178.67
Tuberculoid6131.12
Borderline5528.06
Lepromatous6030.61
Not classified31.51
Educational status
Illiterate94.6
Elementary school9045.9
Incomplete high school3015.3
Complete high school2814.3
Incomplete university or college education52.6
Complete university or college education126.1
Unknown199.7
Not applicable31.5
Bacilloscopy
Positive8040.8
Negative9448.0
Not performed199.7
Unknown31.5
Initial treatment
MDT-PB8141.32
MDT-MB10453.06
Alternative110.51
TOTAL196100%

MDT-PB, paucibacillary multidrug therapy; MDT-MB, multibacillary multidrug therapy.

Table 2

Characteristics of the 56 patients who had adverse effects.

CharacteristicsNumber(%)
Gender
Male2035.71
Female3664.29
Ethnicity
White2748.21
Black814.29
Asian11.79
Mixed-race1832.14
Native Brazilian00
Unknown23.57
Age
00 -1535.36
16 – 452239.28
46 – 691933.93
≥ 701221.43
Clinical presentation
Indeterminate610.71
Tuberculoid1526.79
Borderline2137.50
Lepromatous1323.21
Not classified11.79
Education
Illiterate11.79
Incomplete fourth grade1221.43
Complete fourth grade35.36
Incomplete elementary school58.93
Complete elementary school11.79
Incomplete high school1017.85
Complete high school1017.85
Incomplete university or college education11.79
Complete university or college education610.71
Unknown58.93
Not applicable23.57
Bacilloscopy
Positive2035.71
Negative3053.58
Not performed610.71
Adverse effect dose
First1933.93
Second916.07
Third916.07
Fourth610.71
Fifth or greater1323.21
Initial treatment
MDT-PB2137.50
MDT-MB3562.50
TOTAL56100

MDT-PB, paucibacillary multidrug therapy; MDT-MB, multibacillary multidrug therapy.

Characteristics of the 196 leprosy patients followed-up at the hospital. MDT-PB, paucibacillary multidrug therapy; MDT-MB, multibacillary multidrug therapy. Characteristics of the 56 patients who had adverse effects. MDT-PB, paucibacillary multidrug therapy; MDT-MB, multibacillary multidrug therapy. Most AEs occurred in the first few supervised doses, 33.92% in the first and 76.78% until the fourth (Table 2). DDS was the most implicated drug; it accounted for 96.7% of AE (59/61), and was replaced in almost half of the cases (49.15%). RFP alone represented 3.27% of the AEs and was suspended in only one patient, due to refractory headache. Mild thrombocytopenia occurred in three patients using a combination of RFP and DDS. Some patients presented more than one AE (Table 3).
Table 3

Adverse effects, respective drugs, and suspension.

Adverse effect due to dapsonenDapsone suspension
Chronic hemolytic anemia2411
Acute hemolytic anemia1712
Photosensitivity/photodermatitis22
Methemoglobinemia11
Gastrointestinal manifestation80
Dapsone hypersensitivity syndrome33
Adverse effect due to rifampicinnRifampicin suspension
Gastrointestinal manifestation10
Headache11
Adverse effect due to clofazimine and dapsonenDapsone or clofazimine suspension
Gastrointestinal manifestation10
Adverse effect due to rifampicin and dapsonenDapsone or rifampicin suspension
Thrombocytopenia30
Total adverse effects6130
Adverse effects, respective drugs, and suspension.

Discussion

In the cohort of 196 individuals studied, most MB treatments were in male patients. Nobre et al. reported twice as much MB cases in men (OR = 2.36; 95% CI 2.33–2.38). Half of the patients were between 20 and 40 years of age. Literature data show that AE can occur in up to half of the patients (45%) in MDT; in the present study, it occurred in less than 30%.3, 4, 5 Although more than a quarter (n = 56) of the patients experienced an AE, the drug was replaced in 30 of the 185 cases that started the standard regimen. More than two-thirds of AEs occurred in the first four months of treatment and DDS was the medication most involved, according to reports in the literature. Hematological AE occurred in almost three quarters of the patients and have been related to the individual capacity for sulfamine (DDS) acetylation and hydroxylation. Individuals with hemoglobinopathies, G6PD deficiency, and those receiving oxidative medications may be at increased risk for hemolytic anemia. Dapsone-related photoallergy has led to the discontinuation of the drug in two cases. The occurrence of AE in women was twice as high, corroborating Dupnik's findings of the association of female gender with an increased risk of drug reaction. G6PD genes are on the X chromosome and some mutations lead women with partial disabilities to develop symptoms. In the present study, it was observed that women over 45 years of age had a higher risk of AE, contrary to the findings by Dupnik, who observed it in younger women. The chance of an individual having AE increases with each year of age for both sexes (OR = 1.02; 95% CI 1.00–1.04). Slower metabolization in older patients would justify this finding. Goulart et al. also found an increased risk of hematological effects in older patients. Sulfonic syndrome, although severe, is uncommon; it was observed in 1.53%, in agreement with the literature.3, 5, 10 Gastrointestinal complaints improved with recommendations for concomitant food intake and/or use of antiemetics, not requiring drug suspension.

Conclusions

DDS was responsible for the largest number of AE cases, mainly in the first trimester. Anemia was the most frequent, mainly in women. The risk of AE increases with each year of age. These findings reinforce the need for greater vigilance at the beginning of treatment, in women, and in older patients.

Financial support

None declared.

Authors’ contributions

Violeta Duarte Tortelly: Approval of the final version of the manuscript; design and planning of the study; drafting and editing of the manuscript; collection, analysis, and interpretation of data; effective participation in research orientation; intellectual participation in propaedeutic and/or therapeutic conduct of studied cases; critical review of the literature; critical review of the manuscript. Egon Luiz Daxbacher: Approval of the final version of the manuscript; design and planning of the study; effective participation in research orientation; critical review of the literature. Arles Martins Brotas: Approval of the final version of the manuscript; critical review of the literature; critical review of the manuscript. Sueli Carneiro: Approval of the final version of the manuscript; design and planning of the study; drafting and editing of the manuscript; critical review of the manuscript.

Conflicts of interest

None declared.
  8 in total

1.  Multidrug therapy in geriatric patients.

Authors:  T Oommen
Journal:  Int J Lepr Other Mycobact Dis       Date:  2000-06

2.  Increase in the incidence of dapsone hypersensitivity syndrome--an appraisal.

Authors:  P N Rao; T S Lakshmi
Journal:  Lepr Rev       Date:  2001-03       Impact factor: 0.537

3.  [Adverse effects of multidrug therapy in leprosy patients: a five-year survey at a Health Center of the Federal University of Uberlândia].

Authors:  Isabela Maria Bernades Goulart; Guilherme Leonel Arbex; Marcus Hubaide Carneiro; Mariana Scalia Rodrigues; Rafael Gadia
Journal:  Rev Soc Bras Med Trop       Date:  2002-11-29       Impact factor: 1.581

4.  Hemolysis of red cells due to sulfone.

Authors:  K Mayer; A B Ley
Journal:  Ann Intern Med       Date:  1970-05       Impact factor: 25.391

5.  Adverse effects of multi-drug therapy in leprosy, a two years' experience (2006-2008) in tertiary health care centre in the tribal region of Chhattisgarh State (Bastar, Jagdalpur).

Authors:  Harminder Singh; Bithika Nel; Vivek Dey; Pawan Tiwari; Naveen Dulhani
Journal:  Lepr Rev       Date:  2011-03       Impact factor: 0.537

6.  Intolerance to leprosy multi-drug therapy: more common in women?

Authors:  Kathryn Margaret Dupnik; Fernando José Ramos Cardoso; Ana Luiza Braga Brito De Macêdo; Igor Leonardo Cardoso De Sousa; Renata Cristina Barros Leite; Selma Maria Bezerra Jerônimo; Mauricio Lisboa Nobre
Journal:  Lepr Rev       Date:  2013-09       Impact factor: 0.537

7.  Adverse effects from multi-drug therapy in leprosy: a Brazilian study.

Authors:  Patricia D Deps; Sofia Nasser; Patricia Guerra; Marisa Simon; Rita De Cássia Birshner; Laura C Rodrigues
Journal:  Lepr Rev       Date:  2007-09       Impact factor: 0.537

8.  Multibacillary leprosy by population groups in Brazil: Lessons from an observational study.

Authors:  Mauricio Lisboa Nobre; Ximena Illarramendi; Kathryn Margaret Dupnik; Mariana de Andrea Hacker; José Augusto da Costa Nery; Selma Maria Bezerra Jerônimo; Euzenir Nunes Sarno
Journal:  PLoS Negl Trop Dis       Date:  2017-02-13
  8 in total
  1 in total

Review 1.  A review of nutrition in neuropathic pain of leprosy.

Authors:  Michael Klowak; Andrea K Boggild
Journal:  Ther Adv Infect Dis       Date:  2022-06-01
  1 in total

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