Bipolar disorder: assessment and management

Psychosis and schizophrenia in adults

NICE's full guideline on psychosis and schizophrenia in adults, provides details in the introductory section about the increased risk of diabetes for people with schizophrenia as the rationale for testing for diabetes in this population. Evidence concerning the use of HbA1c, fasting and/or random blood glucose measures for assessing diabetes was not considered during development of this guideline. A rationale for why both HbA1c and fasting blood glucose are recommended for assessing type 2 diabetes before and during treatment with antipsychotics, rather than either HbA1c or fasting blood glucose being recommended (as is the case in the NICE guideline on type 2 diabetes: prevention in people at high risk) is not provided.

Bipolar disorder

NICE's full guideline on bipolar disorder also highlights in the introductory section that bipolar disorder is associated with a higher burden of physical illnesses such as diabetes. The rationale for developing recommendations on diabetes was that 'many guidelines now recommend monitoring of glucose and lipid levels for patients prescribed any antipsychotic ... It is also important to note that many people with bipolar disorder may be at high risk of developing diabetes mellitus and dyslipidaemias resulting from aspects of their lifestyle, irrespective of antipsychotic treatment.'

Recommendations 1.10.5, 1.10.8 and 1.2.12 on measuring HbA1c, fasting and/or random blood glucose were described as adapted from the NICE guideline on psychosis and schizophrenia in adults because 'the GDG (guideline development group) agreed that side effects from antipsychotics will occur in the same way in people with bipolar disorder as they do in people with schizophrenia'. The recommendations were 'adapted by the GDG based on their expertise', no further information for the differences between the 2 guidelines' recommendation content was provided.

Psychosis and schizophrenia in children and young people

NICE's guideline on psychosis and schizophrenia in children and young people (recommendations 1.3.16 and 1.3.19) were made in response to the growing evidence for harmful effects of antipsychotic medications, especially in the young. The GDG considered the underlying evidence and recommendations in NICE's guideline on psychosis and schizophrenia in adults published in 2009 and adapted them.

Antisocial behaviour and conduct disorders in children and young people

NICE's guideline on antisocial behaviour and conduct disorders in children and young people (recommendations 1.6.5 and 1.6.6) on testing fasting blood glucose and HbA1c were also based on NICE's guideline on psychosis and schizophrenia in adults published in 2009.

Acute coronary syndromes

NICE's guideline on acute coronary syndromes (recommendation 1.3.3), states to 'offer all people with hyperglycaemia after acute coronary syndrome and without known diabetes tests for:

These tests should not delay discharge.'

This recommendation was based on evidence from prognostic studies rated as low or very low quality (see hyperglycaemia in acute coronary syndromes [2011 evidence reviews]) that 'showed that both fasting blood glucose and HbA1c could be used to predict diabetes at follow-up' of people with acute coronary syndrome. The GDG 'agreed that patients with high HbA1c levels and fasting blood glucose on discharge were at higher risk of developing diabetes, therefore these tests should be routinely used in practice'. They 'also discussed the fact that blood glucose levels would be distorted as a result of the acute event. Therefore, test results on day 4 may be more reliable than using test results on admission to identify patients who are at higher risk of a diagnosis of diabetes. It was agreed that formal testing and diagnosis of diabetes will normally take place following referral to primary care after the acute episode.'

Recommendation 1.3.7 on advice and ongoing monitoring for people with hyperglycaemia after acute coronary syndrome and without known diabetes says to 'Inform GPs that they should offer at least annual monitoring of HbA1c and fasting blood glucose levels to people without known diabetes who have had hyperglycaemia after an acute coronary syndrome'. It is reported in the evidence review that there was a lack of evidence on the information and support needs of patients with acute coronary syndrome and hyperglycaemia who have no previous diagnosis of diabetes; and that 'there may be variation in terms of which patients are currently provided with follow-up, so the GDG decided that monitoring of this high risk group would be improved by secondary care staff informing the GP that a patient needs routine follow-up. Specifically, it felt that follow-up should include a biochemical test to ensure that diabetes status is assessed'. Reasons for recommending testing both, rather than either HbA1c or fasting blood glucose levels are not detailed.

Type 2 diabetes: prevention in people at high risk

With regards to identifying an adult's risk of developing or having type 2 diabetes, recommendations on risk identification in NICE's guideline on type 2 diabetes: prevention in people at high risk (including identifying prediabetes and type 2 diabetes), say to offer venous blood tests to assess fasting plasma glucose or HbA1c. None of the recommendations discuss the use of random blood glucose testing.

Diabetes (type 1 and type 2) in children and young people: diagnosis and management

Recommendations on diagnosis in NICE's guideline on diabetes (type 1 and type 2) in children and young people say to be aware that signs of type 1 diabetes in children and young people include hyperglycaemia, which is defined as 'random plasma glucose more than 11 mmol/litre'. It recommends that type 1 diabetes in children and young people should be confirmed using the plasma glucose criteria in the World Health Organization's 2006 report on the diagnosis and classification of diabetes mellitus, which provides details on measurements of random and fasting blood glucose for helping in diagnosing diabetes. The full guideline reports that in 'young people with severe symptoms, the diagnosis [of type 1 diabetes] can be confirmed by a random plasma glucose concentration ≥11.1 mmol/l' and says that 'in the unusual situation where a child presents without definitive symptoms but with a plasma glucose concentration ≥11.1 mmol/l, the World Health Organization recommends that a fasting plasma glucose test and/or an OGTT [oral glucose tolerance test] may be required to confirm the diagnosis … a fasting plasma glucose concentration ≥7.0 mmol/l can be used to confirm the diagnosis'. While the GDG agreed with measuring random and fasting blood glucose, they said that 'OGTTs should be discouraged in clinical practice due to their inconvenience, greater cost and lower reproducibility compared with fasting plasma glucose or 2 hours post-glucose plasma glucose tests'.

The guideline recommends that 'when diagnosing diabetes in a child or young person, assume type 1 diabetes unless there are strong indications of type 2 diabetes, monogenic or mitochondrial diabetes' and to 'think about the possibility of type 2 diabetes in children and young people with suspected diabetes who:

The recommendations on diagnosis do not discuss the use of measures of HbA1c or fasting blood glucose for diagnosing type 2 diabetes. The guideline provides recommendations on HbA1c targets and monitoring once a diagnosis of type 2 diabetes has been made.

Clinical knowledge summary on type 2 diabetes in an adult

Clinical knowledge summaries provide primary care practitioners with a readily accessible summary of the current evidence base and practical guidance on best practice. They are not NICE guidance but are hosted on the NICE website. The basis for recommendations on tests for type 2 diabetes are from on multiple sources, including NICE's guideline on type 2 diabetes in adults: management; no other NICE guidelines are referenced.

While the clinical knowledge summary references NICE's guideline on type 2 diabetes in adults: management as a source for advice, this guideline is for adults already diagnosed with type 2 diabetes, and as such is not relevant to the populations being considered in this review, for whom type 2 diabetes has not yet been diagnosed.

The clinical knowledge summary on testing for type 2 diabetes in adults and on diagnosis in children and young people advises that persistent hyperglycaemia in children and young people can be measured by fasting or random blood glucose. It reports that 'the definition of persistent hyperglycaemia is based on Classification of Diabetes Mellitus (WHO, 2019), the ISPAD [International Society for Pediatric and Adolescent Diabetes] clinical practice consensus guidelines (Mayer-Davis et al. 2018; Zeitler et al. 2018), and expert opinion in a review article (Candler et al. 2018). The ISPAD guidelines note that 'no diagnostic criteria have been specifically validated in children and young people and are therefore extrapolated from adult definitions'; and 'the recommendation that HbA1c should not be used to diagnose type 2 diabetes in children and young people is based on the ISPAD clinical practice consensus guidelines (Mayer-Davis et al. 2018) and expert opinion in a review article, which notes that the HbA1c cut-off used to diagnose type 2 diabetes in adults is not considered sufficiently accurate in children to make a diagnosis (Candler et al. 2018)'.