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letter
. 2022 Mar 25;6(1):e36801. doi: 10.2196/36801

Authors’ Reply to: Using Caution When Interpreting Gender-Based Relative Risk. Comment on “The Effect of Cardiovascular Comorbidities on Women Compared to Men: Longitudinal Retrospective Analysis”

Elma Dervic 1,2,#, Carola Deischinger 3, Nina Haug 1,2, Michael Leutner 3, Alexandra Kautzky-Willer 3,4, Peter Klimek 1,2,
Editor: Tiffany Leung
PMCID: PMC8994150  PMID: 35333178

We thank Janszky [1] for their time and observations on our paper [2]. We appreciate the comments.

Our analysis was done on a large data set of hospital diagnoses from 1997 to 2014. We developed a systematic approach to detect all significant gender differences across all comorbidities associated with cardiovascular disease (CVD). In our paper [2], we reported all risk factors and calculated sex differences as a measure of differences using logarithmic odds ratios between male and female patients in units of pooled standard errors. As a limitation, we pointed out that we cannot rule out specific unobserved confounders as well as the limitations of our in-hospital data set. We thank Janszky [1] for providing an illustrative example of how such a confounding influence could work.

It is clear that correlation is not causation, and we did not make any statement on causality. We analyzed the order of diagnoses by conducting a “time directionality analysis,” and our results showed us which diagnoses were “typically diagnosed before.” In the Limitations section, we emphasized this as well: “Given the purely observational nature of our dataset, no statements on causality can be made based on this analysis.” Janszky’s [1] comment clearly shows why it is important to repeatedly stress such limitations.

The motivation behind our work is to increase awareness of the need for gender-specific medicine. It has been well described that the female sex overall is protective in the development of CVD due to biological and psychosocial factors but that metabolic diseases like diabetes attenuate this protective effect [3]. Yet, our knowledge on potential sex-dimorphic pathophysiological mechanisms remains limited, in particular in relation to CVD. With our work, we aim to show how observational data can be used to rapidly generate hypotheses regarding sex differences in disease risk at scale and thereby initiate further research that aims to clarify their potential causal mechanisms.

Abbreviations

CVD

cardiovascular disease

Footnotes

Conflicts of Interest: None declared.

References


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