Sasaki 1982.

Name of study	None
Inclusion criteria	Epidemiological survey on diabetes mellitus in Osaka, Japan and follow‐up study
Exclusion criteria	Not reported
Notes	Baseline data for the IGT cohort (N = 13)
Risk of bias
Bias	Authors' judgement	Support for judgement
Study participation: description of source population or population of interest	Low risk	Yes
Study participation: description of glycaemic status at baseline	Low risk	Yes
Study participation: adequate description of sampling frame & recruitment	Low risk	Yes
Study participation: adequate description of period & recruitment place	Low risk	Yes
Study participation: adequate description of inclusion & exclusion criteria	Unclear risk	Only inclusion criteria described
Study attrition: description of attempts to collect information on participants who dropped out	Low risk	Yes
Study attrition: reasons for loss to follow‐up provided	Unclear risk	Scarce data
Study attrition: adequate description of participants lost to follow‐up	Unclear risk	Scarce data
Study attrition: no important differences between participants who completed the study and those who did not	Low risk	Yes
Glycaemic status measurement: provision of clear definition or description of glycaemic status	Low risk	Yes
Glycaemic status measurement: valid and reliable method of glycaemic status measurement	Low risk	Yes
Glycaemic status measurement: continuous variables reported or appropriate cut points used	Low risk	IGT: FPG < 7.8 and 2‐h PG 7.8–11.1 (WHO 1980)
Glycaemic status measurement: same method and setting of measurement of the glycaemic status for all study participants	Low risk	Yes
Outcome measurement: clear definition of the outcome provided	Low risk	FPG ≥ 7.8 or 2‐h PG ≥ 11.1 (WHO 1980)
Outcome measurement: method of outcome measurement used valid & reliable	Low risk	Yes
Outcome measurement: same method & setting of outcome measurement for all study participants	Low risk	Yes
Study confounding: important confounders measured	Unclear risk	Cumulative incidence
Study confounding: clear definitions of important confounders provided	Unclear risk	Scarce data
Study confounding: measurement of confounders valid & reliable	Unclear risk	Scarce data
Study confounding: same method & setting for measurements of confounders for all study participants	Unclear risk	Scarce data
Study confounding: appropriate methods used if missing confounder data imputed	Unclear risk	Not reported
Study confounding: important potential confounders accounted for in study design	Unclear risk	Cumulative incidence
Study confounding: important potential confounders accounted for in the analysis	Unclear risk	Cumulative incidence, incidence rate
Statistical analysis & reporting: sufficient presentation of data to assess adequacy of the analytic strategy	Low risk	Cumulative incidence
Statistical analysis & reporting: the statistical model is adequate for the design of the study	Unclear risk	Multiple logistic regression (standardised regression coefficients for single covariates)