Frontiers in Public Health (Nov 2020)

Protocol for a Case-Control Study to Investigate the Association of Pellagra With Isoniazid Exposure During Tuberculosis Preventive Treatment Scale-Up in Malawi

  • Scott A. Nabity,
  • Kelvin Mponda,
  • Steve Gutreuter,
  • Diya Surie,
  • Anne Williams,
  • Anne Williams,
  • Andrea J. Sharma,
  • Elizabeth R. Schnaubelt,
  • Rebekah E. Marshall,
  • Hannah L. Kirking,
  • Suzgo B. Zimba,
  • Joram L. Sunguti,
  • Laphiod Chisuwo,
  • Mabvuto J. Chiwaula,
  • Jesse F. Gregory,
  • Robin da Silva,
  • Michael Odo,
  • Andreas Jahn,
  • Thokozani Kalua,
  • Rose Nyirenda,
  • Belaineh Girma,
  • James Mpunga,
  • Nicole Buono,
  • Alice Maida,
  • Evelyn J. Kim,
  • Laurence J. Gunde,
  • Tigest F. Mekonnen,
  • Andrew F. Auld,
  • Adamson S. Muula,
  • John E. Oeltmann

DOI
https://doi.org/10.3389/fpubh.2020.551308
Journal volume & issue
Vol. 8

Abstract

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Background: Pellagra is caused by niacin (vitamin B3) deficiency and manifested by a distinctive dermatitis. Isoniazid is critical for treating tuberculosis globally and is a component of most regimens to prevent tuberculosis. Isoniazid may contribute to pellagra by disrupting intracellular niacin synthesis. In 2017, Malawian clinicians recognized a high incidence of pellagra-like rashes after scale-up of isoniazid preventive treatment (IPT) to people living with HIV (PLHIV). This increase in pellagra incidence among PLHIV coincided with a seasonal period of sustained food insecurity in the region, which obscured epidemiological interpretations. Although isoniazid has been implicated as a secondary cause of pellagra for decades, no hypothesis-driven epidemiological study has assessed this relationship in a population exposed to isoniazid. We developed this case-control protocol to assess the association between large-scale isoniazid distribution and pellagra in Malawi.Methods: We measure the relative odds of having pellagra among isoniazid-exposed people compared to those without exposure while controlling for other pellagra risk factors. Secondary aims include measuring time from isoniazid initiation to onset of dermatitis, comparing niacin metabolites 1-methylnicotinamide (1-MN), and l-methyl-2-pyridone-5-carboxamide (2-PYR) in urine as a proxy for total body niacin status among subpopulations, and describing clinical outcomes after 30-days multi-B vitamin (containing 300 mg nicotinamide daily) therapy and isoniazid cessation (if exposed). We aim to enroll 197 participants with pellagra and 788 age- and sex-matched controls (1:4 ratio) presenting at three dermatology clinics. Four randomly selected community clinics within 3–25 km of designated dermatology clinics will refer persons with pellagra-like symptoms to one of the study enrollment sites for diagnosis. Trained study dermatologists will conduct a detailed exposure questionnaire and perform anthropometric measurements. A subset of enrollees will provide a casual urine specimen for niacin metabolites quantification and/or point-of-care isoniazid detection to confirm whether participants recently ingested isoniazid. We will use conditional logistic regression, matching age and sex, to estimate odds ratios for the primary study aim.Discussion: The results of this study will inform the programmatic scale-up of isoniazid-containing regimens to prevent tuberculosis.

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