Table 2

Recommendations on monitoring including method and interval

	Assessments and feasible methods of monitoring		Minimal monitoring frequency
Adverse event	Clinical trials	Daily practice (if different from clinical trials)	Clinical trials	Daily practice
Cardiovascular
Dyslipidemia	Blood: fasting lipids	–	Start, end	–
Electrolyte disturbances	Blood: sodium and potassium	–	Start, end	–
Edema	Physical examination: ankle edema	–	Start, end	Start
Hypertension	Blood pressure measurement	–	Start, end	Standard care
Ischemic CVD	Questioning Carotid intima-media thickness^*	Questioning	Start, end Start, end^**	Standard care
Infectious
Infections	Questioning: occurrence, treatment with antibiotics	–	Start, during follow-up	–
Gastro-intestinal
Peptic ulcer disease	Questioning: complaints Blood: haemoglobin	–	Start, end Start, end	Standard care
Psychological
Mood disturbances	Questioning	–	Start, end	–
Psychosis	Active monitoring not indicated; report of occurrence	–	–	–
Endocrine and metabolic
Diabetes/glucose intolerance	Blood: fasting glucose and insulin (HOMA)	Blood: fasting glucose	Start, end	Start, standard care
Body weight and fat redistribution	Height Weight Abdominal circumference	Height Weight	Start, end Start, during follow-up Start, end	Standard care
Interference with hormone secretion	Questioning: menstrual disturbances/loss of libido Blood: ACTH stimulation test^*	–	Start, end Start, within 48 h after stopping	–
Dermatological
Skin atrophy	Questioning Sonography for skin thickness (volar part of arm)^*	–	Start, end Start, end^**	–
Acne, hirsutism, alopecia, bruisability	Questioning	–	Start, end	–
Hirsutism	Questioning	–	Start, end	–
Musculo skeletal
Osteoporosis (BMD)	DEXA X-rays dorsal spine (if possible) Questioning for fractures	–	Start, end^** (for newly started GCs: also at six months) Start, end Start, end	Standard care according to local guidelines
Osteonecrosis	Active monitoring not indicated; imaging only in case of complaints	–	–	–
Myopathy	Questioning	–	Start, end	–
Ophthalmological
Cataract	Ophthalmologic evaluation	–	Start, end^**	–
Glaucoma (intra-ocular pressure)	Ophthalmologic evaluation with tonometry	Questioning for risk factors: family history, high myopia, diabetes	Start, end^**	Start (ophthalmologic evaluation in case of risk factors)

↵* This is the preferable monitoring method, but probably less feasible. We ask to incorporate at least one of these items in future trials.
↵** Monitoring is only indicated for studies with a duration of at least 1 year.
For all adverse events (AEs) feasible monitoring methods are described and preferable monitoring intervals are given. These are minimum recommendations, indicating that they can be intensified for patients with additional risk factors for a certain AE. In most cases monitoring is recommended at start and at the end of trials. In case of drop-out, the ‘end’-monitoring should be performed at time of drop-out. Broad explanation about these recommendations is enclosed in Online Appendix 2. In Online Appendix 3 suggestions for questioning are given.
ACTH, adrenocorticotropic hormone; BMD, bone mineral density; CVD, cardiovascular disease; GCs, glucocorticoids; HOMA, homeostasis model assessment.