figure b


Most people with type 2 diabetes and excess body weight have comorbidities such as hypertension, atherogenic dyslipidaemia and non-alcoholic fatty liver disease, contributing to increased disability and mortality [1]. Weight loss improves glycaemic control [2] and ameliorates abnormalities in lipid metabolism [3], which may attenuate risk of microvascular complications [4] and CVD [5], respectively, and may lead to remission of type 2 diabetes [2]. Therefore, lifestyle modification with emphasis on negative energy balance facilitating weight loss is a cornerstone in managing individuals with obesity and type 2 diabetes [6].

Traditionally, an energy-reduced diet rich in fibre, rich in low-glycaemic index carbohydrate and limited in fat (allowing 10–20% of total energy intake from protein) has been the recommended dietary approach in type 2 diabetes treatment [7]. Recently, the ADA concluded in a consensus statement that carbohydrate-restricted dietary regimens may provide viable treatment strategies in the management of type 2 diabetes, although no ideal macronutrient distribution has yet been established [8]. Results from a meta-analysis suggested that low-carbohydrate diets may improve glycaemic control and CVD risk in type 2 diabetes during at least 1 year, even without significant changes in body weight [9].

We recently demonstrated that a 6 week, weight-maintaining, carbohydrate-reduced high-protein (CRHP) diet improved glucose and lipid metabolism and reduced liver fat content compared with a conventional diabetes (CD) diet [10]. However, the clinical utility of low-carbohydrate diets beyond weight loss remains elusive, because these diets often readily decrease body weight despite considerable efforts to prevent this from happening [10, 11], and current dietary regimens for weight loss typically utilise hypo-energetic diets with percentage of total energy intake (E%) >50 from carbohydrate [2, 12]. Accordingly, we investigated the effects of matched weight loss, induced by 6 weeks of hypo-energetic CRHP vs CD feeding, on metabolic health including HbA1c as the primary outcome and liver fat accumulation and circulating triacylglycerol as secondary outcomes in individuals with type 2 diabetes who were overweight or obese.


Study design and population

The study was an open-label, parallel RCT with participants allocated in a 1:1 ratio to a hypo-energetic CD or CRHP diet for 6 weeks. Randomisation was performed in blocks of random size by an unrelated third party using R (extension package ‘blockrand’, Version 3.6.0; R, Boston, MA, USA) to generate a randomisation list.

Eligible participants were adults with BMI >25 kg/m2 diagnosed with type 2 diabetes, an HbA1c of 48–97 mmol/mol (6.5–11.0%), and who were receiving glucose-lowering therapy restricted to metformin or dipeptidyl peptidase-4 (DPP-4) inhibitors. Initial inclusion criteria for HbA1c (>53 mmol/mol [7.0%]) and BMI (>27 kg/m2) were lowered prior to study initiation to facilitate recruitment. Exclusion criteria were as follows: previous cancer and heart failure; recent and ongoing ischaemic heart disease; severe disease of the liver, kidneys and alimentary tract; anaemia (blood haemoglobin <7 mmol/l for men and <6 mmol/l for women); renal dysfunction (eGFR <30 ml min−1 [1.73 m]−2 or urine albumin/creatinine ratio >300 mg/g); inability to comply with study procedures; participation in other studies; lactation; pregnancy (or planning a pregnancy); treatment with systemic corticosteroids, sulfonylureas, sodium–glucose cotransporter 2 inhibitors or injectable hypoglycaemic medications; alcohol abuse, defined as consumption in excess of national recommendations (<168 g/week for men and <84 g/week for women); and smoking during the past year. Participants were recruited from the Capital Region of Denmark from January 2019 to July 2020 and all visits took place at the Endocrinology Research Unit, Copenhagen University Hospital Bispebjerg, except for magnetic resonance (MR) assessments that were performed at Copenhagen University Hospital Herlev. Participants provided written, informed consent to the study protocol, which was approved by the Health Ethics Committee of Copenhagen and the Danish Data Protection Agency. The study is registered with (registration no. NCT03814694) and was conducted in accordance with the Declaration of Helsinki.

Diet intervention

The control CD diet and experimental CRHP diet differed in macronutrient composition, and respectively provided 50E% and 30E% as carbohydrate, 17E% and 30E% as protein, and 33E% and 40E% as fat (electronic supplementary material [ESM] Table 1). Study diets provided all daily energy and comprised seven different daily menus, with three main meals per day with or without two snacks (ESM Table 2). Raw food items and ingredients were used to prepare the various meals and snacks, which were cooked and provided to the participants ready for consumption. All meals were prepared in the metabolic kitchen at the Department of Nutrition, Exercise and Sports, University of Copenhagen and were distributed free-of-charge, twice weekly.

Participants were instructed to consume all meals and abstain from all alcohol- and energy-containing beverages as well as any food not provided by the investigators. Dietary adherence was evaluated twice weekly by using food records. In case of inability to consume all provided food (e.g. due to satiety or aversion), individual adjustments were made. Participants were asked prior to inclusion about food allergies, fastidiousness and dietary preferences and were excluded if their responses conflicted with compliance to the study diets.

Weight loss management

Dietary regimens were designed to induce the same energy deficit during the first 5 weeks of the intervention period in order to achieve a 6% weight loss. During week 6, energy intake was adjusted upwards to ensure stabilisation at the new lower body weight and avoid a catabolic state during metabolic measurements. Weight loss management was individualised to each participant and occurred in three steps (ESM Table 3). First, total energy expenditure (TEE) was calculated by multiplying resting energy expenditure, estimated from the Mifflin–St Jeor equation [13], with a physical activity level of 1.6, reflecting a sedentary lifestyle. Second, the total energy equivalent of weight loss was calculated as 6% of baseline body weight × 27,000 kJ/kg (6453 kcal/kg), as we expected lost weight to comprise ~75% adipose tissue and ~25% lean mass [14]. Daily energy intake was then calculated as TEE reduced by an amount equal to the total energy equivalent of weight loss divided by the total duration of the weight-loss phase (i.e. 35 days). The calculated reduction was weighted with 80% initially and gradually increased to 120% at week 5 to allow for habituation. Third, the planned energy deficit was revisited twice weekly (based on body weight measurements) and adjusted as necessary by adding or subtracting CRHP or CD food items to ensure the targeted weight loss. Participants were instructed to maintain their habitual physical activity throughout the study. This was assessed at baseline and during week 5 of the intervention with the long form of the International Physical Activity Questionnaire (IPAQ) [15].

Anthropometry and body composition

Body weight measurements were performed, after participants had fasted for 10 h, on the same calibrated digital scale (Seca 701; Hamburg, Germany) at every visit. Assessment of body composition was performed at the beginning and the end of the study, after participants had fasted for 10 h, by use of a Lunar iDXA dual-energy x-ray absorptiometry scanner (GE Healthcare, Waukesha, WI, USA).

Blood samples

Blood samples were collected, after participants had fasted for 10 h, at baseline and weeks 2, 4, 5 and 6. Blood was collected in precooled EDTA-tubes and immediately centrifuged to separate plasma, and in tubes with clot activator, allowed to clot at room temperature, and centrifuged thereafter to separate serum. Measurement of HbA1c was performed using HPLC on the Tosoh Automated Glycohemoglobin Analyzer HLC-723G8 (Tosoh Corporation, Japan). Plasma glucose was measured using the glucose oxidase method (YSI 2300 STAT Plus; YSI, OH, USA) and serum insulin and C-peptide were measured using electrochemiluminescence immunoassays (Cobas 6000 e601; Roche Diagnostics, Switzerland). Whole-body insulin resistance (HOMA2-IR) was calculated from fasting plasma glucose and insulin concentrations by using the updated HOMA2 calculator (version 2.2.3; Total cholesterol, LDL-cholesterol, HDL-cholesterol and triacylglycerol concentrations were determined in serum by enzymatic colorimetric methods, and apolipoprotein (apo) B, apoA-1 and cystatin C were measured by immunoturbidimetric assays (Cobas 6000 c501; Roche Diagnostics). Non-HDL-cholesterol was calculated by subtracting HDL-cholesterol from total cholesterol. Cystatin C was used in the Chronic Kidney Disease Epidemiology Collaboration (CKD-EPI) equation from 2012 to calculate eGFR, by which renal function can be reliably assessed without confounding from changes in protein intake or body composition [16]. Serum total NEFA were quantified with an enzymatic colorimetric assay (Wako Chemicals, Germany).


MR measurements were conducted at the beginning and the end of the study using a 3.0 T Ingenia MRI system (Philips Healthcare, Best, the Netherlands) with a dStream torso coil. Single-voxel MR spectroscopy (Point RESolved Spectroscopy [PRESS]) was used to measure total hepatic and muscle fat fractions [17]. Chemical shift encoding-based water-fat imaging (mDixon) was used to measure pancreatic fat fraction, visceral adipose tissue (VAT), subcutaneous adipose tissue (SAT) and waist circumference. Pancreatic fat content was measured in duplicates, and the mean was used to minimise intra-observer variability. A single 10 mm thick transverse section acquired at the middle of L3 vertebra was used for quantification of VAT, SAT and waist circumference [18]. All MR data were analysed blinded to treatment.

Diurnal glucose profiles

The diurnal glucose profiles were obtained from measurements over 7 days at baseline before the intervention and during the last week (week 6) of the intervention by continuous glucose monitoring (CGM) using the FreeStyle Libre Pro (Abbott Diabetes Care, Alameda, CA, USA), which provides subcutaneous interstitial glucose, blinded to the participant, every 15 min. The glucose monitor was pre-calibrated and inserted a day prior to starting the measurement period. Data were evaluated as mean glucose, glucose CV, time-in-range (3.9–10 mmol/l) as well as time above/below range [19]. The variables were calculated for each 24 h period (midnight to midnight) and included in the analyses as the mean of monitored days.

Urine samples

Twenty-four hour urine specimens were collected prior to the intervention and during week 5 of the intervention to determine the excretion of urea as a marker of protein intake and, thus, a marker of diet compliance [20], and albumin as a marker of renal function. Urea was analysed by kinetic testing with urease and glutamate and albumin by immunoturbidimetric analysis (Cobas c6000; Roche Diagnostics). Albumin values <0.05 μmol/l (detection limit) were set to 0.025 μmol/l.

Statistical analysis

The primary outcome was the change in HbA1c between diet groups; secondary outcomes were changes in hepatic fat content and serum triacylglycerol. The protocol included 47 additional pre-specified outcomes of which 16 are presented in this paper (ESM Table 4). On the basis of treatment effect differences between weight-maintaining CRHP and CD diets [10] and a significance level of 0.05, we estimated that 21 participants in each group (total of 42 participants) would be required to detect an HbA1c difference of 5.4 mmol/mol (0.5%) between groups, with 90% power providing an SD of 5.2 mmol/mol (0.4%), whereas a 3.6% difference in liver fat (SD 4.8%) could be detected with 29 participants per group (total of 58 participants) with 80% power. After accounting for a smaller than expected effect size and an anticipated 20% dropout rate, a final sample size of 80 participants was computed.

Treatment effects were evaluated using a constrained linear mixed model with inherent baseline adjustment and further assuming an unstructured covariance pattern to account for repeated measurements. Moreover, sensitivity analyses were conducted to further adjust for differences in sex, age, BMI, diabetes duration, and therapy with metformin and DPP-4 inhibitors. In accordance with an intention-to-treat principle, analyses included all available data and missing data were implicitly managed by maximum likelihood estimation, which is statistically optimal when missing data are assumed to be missing at random. Model assumptions were assessed from residual diagnostics and skewed outcomes were log-transformed prior to analysis. Between-diet comparisons are presented as estimated marginal means (95% CIs), unless otherwise stated. Descriptive data are reported as mean ± SD or median (25th, 75th percentile), depending on whether normal distribution assumptions were met or not, assessed visually and evaluated by the Shapiro–Wilks test.

Statistical tests were two-tailed and considered significant when p < 0.05. All statistical analyses and graphics were performed using R (Version 3.6.0; R, Boston, MA, USA).


Study flow and participants

The recruitment process included 338 pre-screenings and 102 on-site screening visits; 72 participants were finally included in the study. Two participants withdrew consent before the start of the study and three after starting the intervention, resulting in an attrition rate of 6.9% (CD 8.3%, CRHP 5.6%). Reasons for withdrawal were not related to adverse events or trial outcomes (Fig. 1). Because of restrictions due to the COVID-19 pandemic, 72 participants rather than the planned 80 were included in the study, with 67 completers securing statistical power to assess primary and secondary outcomes. Baseline characteristics were well balanced between groups (Table 1), except for a higher proportion of participants allocated to the CRHP diet group being male and being treated with DPP-4 inhibitors compared with the CD diet group. Metformin, DDP-4 inhibitors and all medications known to lower lipids and BP were stable for at least 2 months prior to study initiation and were kept unchanged throughout the study. Study results were not materially altered when adjusted for differences in diabetes medication and other relevant covariates (ESM Table 5).

Fig. 1
figure 1

Participant flow diagram. The median (25th, 75th percentile) time from randomisation to initiation of dietary intervention upon which participants were unblinded was 22 (18, 30) days for the CRHP diet and 22 (19, 31) days for the CD diet

Table 1 Baseline characteristics of study participants

Body weight, anthropometry and body composition

Both interventions reduced body weight by a mean of 5.8 kg (Table 2) and this was successfully maintained during the last week (Fig. 2a). Waist circumference, body fat per cent, fat mass and fat-free mass decreased significantly in both groups without significant differences between diets. The energy intake gradually decreased from ~7900 kJ/day during week 1 to ~6300 kJ/day during week 5 of the intervention (i.e. before the weight maintenance week) (ESM Table 1), with no difference overall between diets (19 [−624, 662] kJ/day, p = 0.95).

Table 2 Measures of anthropometry, body composition and fat distribution before and after matched weight loss by a CD or a CRHP diet in individuals with overweight or obesity and type 2 diabetes
Fig. 2
figure 2

Fasting measures of body weight (p = 0.83) (a), HbA1c (p = 0.018) (b), plasma glucose (p = 0.64) (c), serum insulin (p = 0.92) (d) and serum triacylglycerol (TAG) (p < 0.01) (e) during 6 weeks of a CRHP (n = 34) or CD (n = 33) diet. Data are presented as mean with SEM error bars, including back-transformed data in (ce) following log-transformation. Changes from baseline to week 6 were evaluated between diets, and p values for these differences are included

Ectopic fat deposition

Hepatic fat content was reduced significantly by 51% and 64% after the CD and CRHP diet, respectively, with the difference between groups reaching borderline significance (−26 [−45, 0]%, p = 0.051) (Table 2). Pancreatic fat content decreased with both diets but to a significantly smaller extent by the CRHP diet when compared with the CD diet (33 [7, 65]%, p = 0.010), while the muscle fat fraction did not change on either diet despite weight loss. Volumes of VAT and SAT were reduced significantly and similarly in the two diet groups.

Glycaemic control and metabolic variables

HbA1c was reduced after weight loss in both groups, and reductions were significantly greater with the CRHP than the CD diet (−1.9 [−3.5, −0.3] mmol/mol (−0.18 [−0.32, −0.03]%), p = 0.018) (Table 3, Fig. 2b). Fasting glucose (Fig. 2c), insulin (Fig. 2d), C-peptide and HOMA2-IR decreased to the same extent in both diet groups. Furthermore, when compared with the CD diet, the CRHP diet reduced fasting triacylglycerol concentration by 18 (6, 29)% (p < 0.01) (Fig. 2e). The changes in fasting NEFA, apoB, apoA-1, total cholesterol, LDL-cholesterol, HDL-cholesterol and non-HDL-cholesterol concentrations were similar between diets, and all lipid variables except for NEFA decreased significantly with weight loss (Table 3 and ESM Fig. 1).

Table 3 Measures of glucose and lipid metabolism and CGM before and after matched weight loss by a CD or a CRHP diet in individuals with overweight or obesity and type 2 diabetes


CGM data were available (median [25th, 75th percentile]) for 7 (7, 7) days both at baseline and at 6 weeks in both intervention groups. Both groups achieved improved glucose profiles after weight loss compared with the baseline habitual diet (Table 3). However, the reduction in diurnal mean glucose and glucose CV was greater after the CRHP diet than the CD diet by −0.8 (−1.2, −0.4) mmol/l (p < 0.001) and −4.1 (−5.9, −2.2)% (p < 0.001), respectively. Additionally, although the time-in-range did not significantly differ between groups, participants randomised to the CRHP diet spent significantly less time above 10.0 mmol/l (−3.5 [−6.4, −0.6]%, p = 0.019) and significantly more time below 3.9 mmol/l (8.1 [2.4, 13.9]%, p < 0.01) throughout the day. The participants randomised to the CRHP diet were also more inclined to have CGM-determined hypoglycaemia (i.e. one CGM reading <3.9 mmol/l) (CD 70%, CRHP 82%), including glucose values <3.0 mmol/l (CD 9%, CRHP 29%) (p = 0.24 and p = 0.06, respectively, by Fisher’s Exact test), compared with those randomised to the CD diet.

Renal function and compliance measures

No differences between diets were found in eGFR (5.3 [2.9, 13.5] ml min−1 [1.73 m]−2, p = 0.21), 24 h total albumin excretion (28 [−4, 69]%, p = 0.090), or albumin/creatinine ratio (19 [−10, 58]%, p = 0.23) (ESM Table 6). The CRHP diet increased daily urea excretion (184 [140, 229] mmol, p < 0.001) compared with the CD diet, consistent with a higher protein intake. Physical activity levels were not different between groups (0 [−27, 37]%, p = 0.99) and were unchanged from baseline. However, according to the scoring protocol, 14 inadequately or erroneously answered questionnaires were excluded from the analysis.

Adverse events

Participants were asked about any adverse events at study visits at baseline and weeks 2, 4, 5 and 6 and instructed to contact the study personnel in case of serious adverse events. Thirteen participants (CD 5, CRHP 8) experienced symptoms of mild constipation, which were remedied by sufficient fluid intake and laxatives (CD 2, CRHP 7), including one severe case of obstipation (CRHP). Other symptoms were episodes of diarrhoea (CD 2, CRHP 2), episodes of dizziness (CD 1, CRHP 2) and increased tiredness or lack of energy (CD 0, CRHP 2). One participant (CRHP) experienced transient episodes of excessive sweating with increasing plasma creatinine, although no underlying medical cause could be identified. Despite the CGM-determined time spent below 3.9 mmol/l and the number of hypoglycaemia events being greater for participants on the CRHP diet, all hypoglycaemic events were asymptomatic and no episodes of severe hypoglycaemia as defined by the ADA [21] occurred.


A clinically relevant weight loss induced by a CRHP diet resulted in greater improvements in HbA1c and diurnal glucose profile when compared with a matched weight loss induced by a CD diet in individuals with type 2 diabetes. The CRHP diet also lowered fasting triacylglycerol concentrations and hepatic fat content to a greater extent than the CD diet. Nevertheless, weight loss per se was, as expected, highly effective in improving metabolic health.

Weight loss achieved by a standard diabetes diet has been shown to ameliorate abnormalities in glucose metabolism and decrease HbA1c [2, 12], particularly when at least 5% of initial body weight is lost [3]. While both diet groups in the present study achieved reductions in HbA1c levels during weight loss, the CRHP diet reduced HbA1c levels significantly more than the CD diet. This indicates that better glycaemic control can be achieved independent of weight loss by dietary carbohydrate restriction, although differences in other macronutrients (e.g. protein or monounsaturated fat) may have contributed [22]. Nevertheless, these improvements in HbA1c may be modest during energy restriction compared with iso-energetic feeding [10], underlying the primary importance of weight reduction over macronutrient composition. Iso-energetic meals with lower carbohydrate content acutely attenuate postprandial glucose and insulin excursions in type 2 diabetes, thus decreasing daily mean glucose [23, 24]. We made a similar observation during 6 weeks of a weight-maintaining CRHP diet that led to reduced HbA1c compared with an iso-energetic CD diet [10]. Fasting glucose and insulin concentrations in the present study were equally reduced by the two diets. Diurnal mean glucose decreased significantly more with the CRHP diet, thus the greater reduction in HbA1c has likely resulted from the persistent reductions in postprandial glucose excursions following the CRHP meals. Less carbohydrate being ingested with the CRHP meals compared with the CD meals may primarily drive the reductions in postprandial hyperglycaemia [23].

Diurnal glucose profiles are considered as supplementary to HbA1c in evaluating the quality of glucose control; this includes time-in-range and glucose excursions as independent therapy targets [19, 21]. Exacerbated glucose excursions measured as glycaemic variability (e.g. glucose CV) are progressively being considered as an independent CVD risk factor [25] and are readily attenuated in individuals with type 2 diabetes by carbohydrate restriction, even when in net energy balance [26]. We demonstrate here that reducing carbohydrate intake is beneficial even during hypo-energetic feeding and weight loss. The additional beneficial effects of carbohydrate restriction on hyperglycaemia and glycaemic variability could be of clinical importance and may persist even in combination with other lifestyle interventions [27].

Type 2 diabetes is often accompanied by excess accumulation of intrahepatic fat [28]. The pathogenesis of fatty liver disease involves abnormally increased hepatic de novo lipogenesis (DNL) in concert with elevated peripheral NEFA flux and a channelling of intrahepatic fatty acids towards storage [29]. Hyperinsulinaemia and hyperglycaemia augment hepatic DNL and contribute to liver fat accumulation and hypertriacylglycerolaemia [30], which can further elevate circulating NEFA levels through ‘spill-over’ during lipoprotein-bound triacylglycerol hydrolysis in the periphery [29]. We speculate that reversal of these processes by weight loss is responsible for much of the observed decreases in intrahepatic fat. Alcohol abstinence during the study may have exaggerated these decrements in both diet groups; however, a substantial contribution is unlikely given that none of the participants had a habitual alcohol abuse.

The greater decrease in liver fat with the CRHP diet than the CD diet may be responsible for the greater reduction in circulating triacylglycerol. In fact, we recently demonstrated that accumulation of liver fat in type 2 diabetes can be effectively reduced, in concert with fasting triacylglycerol levels, by iso-energetic substitution of carbohydrate by protein and fat during weight-stable conditions [10], and another study showed the same after iso-energetic substitution of carbohydrate by monounsaturated fat [31]. As such, our results may have been influenced by the higher intake of protein or monounsaturated fat in the CRHP diet [32]. Our finding is at odds with previous studies in overweight and obese individuals without diabetes, in which a moderate weight loss (~7% of baseline body weight) induced by low-carbohydrate and low-fat diets decreased liver fat to the same extent [33, 34]. However, it has been speculated that the presence of diabetes may fundamentally enhance the efficacy of carbohydrate restriction during both weight stability and weight loss [32].

It is difficult to evaluate the clinical relevance of the greater reduction in pancreatic fat content after the CD diet than after the CRHP diet. Studies evaluating intrapancreatic fat in relation to glucose metabolism and beta cell function in individuals with type 2 diabetes are scarce and provide conflicting data, possibly due to the largely heterogenous distribution of fat within the pancreas [35]. Nevertheless, reductions in pancreatic fat accumulation are thought to be important for recovery of pancreatic insulin secretion and, subsequently, for weight loss-induced remission of type 2 diabetes [36]. Our findings should thus be confirmed in future studies.

The long-term safety of carbohydrate restriction also needs to be considered as some people with type 2 diabetes are vulnerable to low-carbohydrate diet-induced hypoglycaemia [37]. The present study substantiates this concern, as participants randomised to the CRHP diet had significantly more CGM readings below 3.9 mmol/l. Care should thus be taken, particularly in individuals already at risk of hypoglycaemia (e.g. those receiving insulin or sulfonylurea). Increased protein intake has also been scrutinised in diabetic kidney disease as a possible cause of further renal dysfunction [38], although individuals without overt kidney disease do not seem to be adversely affected [27].

Our study has several strengths including the standardised and tightly controlled intervention that involved full provision of the experimental diets and regular visits to maximise compliance, minimise attrition and achieve the same rate and amount of weight loss between groups. We found a high degree of adherence to the provided diets as indicated by the 65% greater 24 h urinary urea excretion on the CRHP diet (corresponding to the 76% greater dietary protein content) compared with the CD diet, even though the utility of this index during energy restriction and negative nitrogen balance may be limited [20]. Matching energy deficits and weight loss between groups is important because energy restriction and small differences in weight loss have been recognised as important confounders in trials of low-carbohydrate diets [32, 39].

Our study is limited by the unblinded design and the imbalance of sex distribution and use of DPP-4 inhibitors between groups. We did not objectively evaluate physical activity, even though we used a self-reported tool that revealed no changes during the intervention and no differences between groups. The duration of our study was limited to 6 weeks, which is half the time required for HbA1c reductions to achieve a new steady state. However, as HbA1c levels decreased linearly with time during the CRHP diet (as shown previously during 10 weeks on a similar CRHP diet [40]) and the difference between our groups became progressively greater, the effect size following 2–3 months would likely have been greater than the one reported here after 6 weeks. This assertion is supported by the larger improvement in mean diurnal glucose, by 0.8 mmol/l (~50%), after the CRHP diet than after the CD diet. Another limitation relates to multiple testing, which without adjustment increases the risk of false-positive findings. Therefore, interpretation of the results for secondary and exploratory outcomes in the present study should be made with caution and our results should be confirmed in future studies. Finally, our study allowed the quality of dietary carbohydrate, protein and fat to vary naturally, reflecting the real foods used, and dietary components such as fibre (higher in the CD diet) and monounsaturated fat (higher in the CRHP diet) may have affected glycaemic control [22, 41, 42] and hepatic fat accumulation [31] independently of the macronutrient distribution.

In accordance with our results, some studies provide evidence of beneficial short-term effects of substituting carbohydrate with either protein or fat on glycaemic control and blood lipid profile in individuals with type 2 diabetes [9, 39]. However, meta-analyses are inconclusive regarding long-term benefits [9, 39] and, accordingly, conclusions from the recent consensus statement [8] on the efficacy of carbohydrate restriction remain ambiguous. Nonetheless, this may be related to decreasing dietary adherence over time [37, 39] or to heterogeneity among the included studies with respect to the composition and quality of dietary macronutrients, and differences in the amount of weight loss and concurrent exercise training. Adherence to low-carbohydrate diets may be particularly challenging when carbohydrate is severely restricted, whereas more moderate restrictions may be easier to comply with [37]. We have previously shown that individuals with type 2 diabetes can effectively migrate from full CRHP diet provision to a self-selected and self-prepared CRHP dietary pattern for at least 6 months in free-living conditions [43]. Before an optimal diet composition can be recommended, future studies should address long-term efficacy, feasibility and safety of different eating patterns, irrespective of concurrent lifestyle modification, as well as their additive or synergistic effects with weight loss [8].

In conclusion, a 6% weight loss induced by a CRHP diet over 6 weeks modestly improved HbA1c, diurnal glucose, circulating triacylglycerol and liver fat to a greater extent than the same amount of weight loss induced by a CD diet. These findings indicate that during matched weight loss, moderate carbohydrate restriction with subsequent increases in protein and fat can modestly improve metabolic health in individuals with obesity and type 2 diabetes, at least in the short-term. This may be relevant when designing dietary strategies for the management of type 2 diabetes.