Use of Mendelian Randomization to assess the causal status of modifiable exposures for rheumatic diseases, 2024, Zhao et al

Use of Mendelian Randomization to assess the causal status of modifiable exposures for rheumatic diseases

Sizheng Steven Zhao, Stephen Burgess

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Abstract
The explosion in Mendelian randomization (MR) publications is hard to ignore and shows no signs of slowing. Clinician readers, who may not be familiar with jargon-ridden methods, are expected to discern the good from the many low-quality studies that make overconfident claims of causality or stretch the plausibility of what MR can investigate.

We aim to equip readers with foundational concepts, contextualized using examples in rheumatology, to appraise the many MR papers that are or will appear in their journals. We highlight the importance of assessing whether exposures are under plausibly specific genetic influence, whether the hypothesized causal pathways make biological sense, and whether results stand up to replication and use of control outcomes.

Quality of research can vary substantially using MR as with any design, and all methods have inherent limitations. MR studies have provided and can still contribute valuable insights in the context of evidence triangulation.

Link | PDF (Best Practice & Research Clinical Rheumatology) [Open Access]

 

This is an accessible overview of what limitations to be aware of with MR studies.

One of the main things they stress is that there should be a plausible connection between the genetic variant and the exposure. Ideally there is some direct mechanistic connection between the gene and the exposure of interest. Using genes that were obtained from a GWAS that are simply associated with an exposure have much more potential to violate the assumptions of MR, even when the typical statistical tests indicate no violations.

[Edit: changed wording] They say it is good to check if researchers used the MR-STROBE checklist.