Sample description

For this study, we recruited a total of 49 female participants. The final sample consisted of 47 individuals (n = 22 recAN and n = 25 HC) who completed both study sessions (i.e. ATD and sham depletion). Two HC dropped out between the two sessions (n = 1 due to subjective intolerance of the ATD procedure and n = 1 due to scheduling difficulties). To be considered ‘recovered’, participants had to (1) maintain a body mass index (BMI) of >18.5 (age 19 to 29) or be above the 10^th BMI percentile with respect to their age (age 12 to 18; Kromeyer-Hauschild et al., Reference Kromeyer-Hauschild, Wabitsch, Kunze, Geller, Geiß, Hesse and Korte2001) for at least 12 months, (2) menstruate, and (3) refrain from binging, purging or other substantially restrictive eating patterns. The control group consisted of normal-weight, eumenorrhoeic women with no history of psychiatric illness. We generally excluded participants if they had a lifetime history of any of the following clinical diagnoses: bulimia nervosa or binge eating disorder, schizophrenia, substance dependence, bipolar disorder and suicidality. Further exclusion criteria for all participants were incomplete ATD drink intake, nausea or other related intolerance of the ATD mixture, IQ lower than 85, organic brain syndrome, chronic medical or neurological illnesses that could affect appetite, eating behavior or body weight (e.g. diabetes), pregnancy, breast feeding, use of psychotropic medications or substances within the 4 weeks preceding the study. See Supplemental Material 1 (SM 1) for a full list of exclusion criteria.

This study was approved by the ethics committee of the Technische Universität Dresden and carried out in accordance with the latest version of the Declaration of Helsinki, and all participants (and their guardians if underage) gave written informed consent.

Clinical measures

For all participants, the presence or absence of current diagnoses of eating disorders was ascertained by evaluation of the expert form of the Structured interview of AN and bulimia nervosa (SIAB-EX; Fichter & Quadflieg, Reference Fichter and Quadflieg1999). Additionally, a structured clinical interview (Mini-DIPS; Margraf, Reference Margraf2013) was used to rule out other active psychiatric disorders. Interviews were conducted by clinically experienced and trained research assistants under the supervision of the attending child and adolescent psychiatrist.

In addition to the clinical interviews, eating disorder-specific psychopathology was assessed with the German version of the Eating Disorders Inventory (EDI-2; Paul & Thiel, Reference Paul and Thiel2005). Furthermore, depressive symptoms were examined using the Beck Depression Inventory II (BDI-II; Hautzinger, Kühner, & Keller, Reference Hautzinger, Kühner and Keller2009). IQ was assessed with a short version of the German adaption of the Wechsler Adult Intelligence Scale (von Aster, Neubauer, & Horn, Reference von Aster, Neubauer and Horn2006). BMI standard deviation scores (BMI-SDS) were calculated for each participant, which is controlled for both age and sex (Kromeyer-Hauschild et al., Reference Kromeyer-Hauschild, Wabitsch, Kunze, Geller, Geiß, Hesse and Korte2001).

Procedure

The ATD procedure entailed a double-blind, randomized crossover design with each participant undergoing both the depletion and the sham depletion within a period of 7–14 days to avoid potential carry-over effects (M = 9.64, s.d. = 3.21). On the day prior to the study appointments, participants were asked to restrict meals to low protein food and given a list with meal suggestions. Immediately before the ATD and sham depletion intake at 8.30 a.m., participants were weighed. The ATD and sham depletion drinks were then prepared using a weight-adapted dosing regimen (Moja et al., Reference Moja, Stoff, Gessa, Castoldi, Assereto and Tofanetti1988; Zepf et al., Reference Zepf, Sánchez, Biskup, Kötting, Bubenzer, Helmbold and Kuhn2014; for a more detailed description of the ATD mixture, see the Supplements 2). After the ATD/sham depletion intake, participants were given a TRP free breakfast. 4 h after the ATD/sham depletion intake, the MRI session was performed. Participants were continuously supervised by trained staff.

Biochemical measures

Blood samples were taken before the ATD/sham depletion intake as well as approximately 5 h later immediately after the MRI session using a venous catheter (Braunüle®) and ethylenediaminetetraacetic (EDTA) tubes (Sarstedt, Germany). For more details on the biochemical measures and analyses, see SM 3.

To quantify the depletion effect, the ratio of plasma TRP to LNAAs (namely valine, methionine, isoleucine, leucine, phenylalanine, thyrosine) was calculated for each participant using the values of the blood samples immediately after the MRI session (5 h after ATD or sham depletion intake).

Instrumental motivation task

During the fMRI session, participants performed the same instrumental motivation task (Bühler et al., Reference Bühler, Vollstädt-Klein, Kobiella, Budde, Reed, Braus and Smolka2010; Kroemer et al., Reference Kroemer, Guevara, Ciocanea Teodorescu, Wuttig, Kobiella and Smolka2014) that we have used in previous studies in both acute (Steding et al., Reference Steding, Boehm, King, Geisler, Ritschel, Seidel and Ehrlich2019) and weight-recovered (Ehrlich et al., Reference Ehrlich, Geisler, Ritschel, King, Seidel, Boehm and Kroemer2015) AN samples. In addition to allowing for measurement of event-related brain activity in response to stimuli predicting monetary reward (reward anticipation) and feedback about the magnitude of the reward received, this particular task variant has the advantage of providing behavioral assessment of motivation operationalized as instrumental responding (number of button presses, #bp) to maximize reward. Each trial included an anticipation phase, a motor response phase, and a feedback (receipt) phase (Fig. 1 for details). The scanning session started with an eight-trial test run to determine each individual's maximum #bp. This information was used to standardize the cumulative monetary gain to ≈ €10 in the subsequent main run, irrespective of inter-individual performance differences in motor speed (for more information, see SM 4).

Fig. 1. Instrumental motivation task. Instrumental motivation task during event-related functional MRI (fMRI). During the anticipation phase a visual cue was presented for 3 s to inform the participant about the reward level of this trial [reward levels: 0 (no reward), 1, 10, 100]. The motor (or instrumental) response phase started after a 2 s fixation period. Monetary reward per trial increased with reward level and higher effort and was determined by multiplying number of button presses × reward level × an individual adjustment factor (calculated based on the individual maximum #bp in the test run; for details see Bühler et al., Reference Bühler, Vollstädt-Klein, Kobiella, Budde, Reed, Braus and Smolka2010). Acoustic feedback for button presses was provided through headphones. After another fixation period of 4 s, feedback was provided for 3 s by displaying the amount of money gained in this trial and the cumulative amount. Between trials, participants fixated on crosshairs for 3 s (75%) or 7.44 s in 25% of all trials, which improves design efficiency by jittering. The fMRI main run had a total duration of 15.5 min and comprised 48 trials in total (4 reward levels × 12 pseudorandomized repetitions).

Instrumental response data analysis

We compared average #bp and reaction times (RT) of initial responses at each reward level between recAN and HC participants using linear mixed-effects models for the analysis of repeated measurement treating participants as random effects. We assumed a compound symmetry covariance structure for changes of instrumental response by reward level (0, 1, 10, 100) and included group (recAN, HC) and individual TRP/LNAA ratios as indicators of the ATD condition as factors as well as interaction effects (slope) between all variables. Since the variable indicating reward level was centered (and HC were used as a reference for the factor group) the intercept in HC (and intercept + main effect of group in recAN) represents not instrumental responses at reward level 0 but the ‘typical’ response, i.e. it correlates highly with the response rate at an average reward level.

Structural and functional image acquisition, data processing and analysis

Images were acquired using standard sequences with a 3 T whole-body MRI scanner (TRIO; Siemens, Erlangen, Germany) equipped with a standard head coil (SM 5). Functional and structural images were processed with SPM8 (http://www.fil.ion.ucl.ac.uk/spm) within the Nipype framework (http://nipy.sourceforge.net/nipype/; Gorgolewski, Storkey, Bastin, & Pernet, Reference Gorgolewski, Storkey, Bastin and Pernet2012) following standard procedures (SM 6). We evaluated fMRI data quality by manual inspection and using the artifact detection tool (ART; Whitfield-Gabrieli et al., Reference Whitfield-Gabrieli, Thermenos, Milanovic, Tsuang, Faraone, McCarley and Seidman2009). Volumes that exceed an intensity threshold of three standard deviations or a threshold of 2 mm normalized movement in any direction were classified as outliers and excluded from statistical models (motion-outlier: recAN individuals, day 1: 2.47 ± 10.31, day 2: 0.35 ± 0.87; HC, day 1: 0.05 ± 2.13, day 2: 0.18 ± 0.66; intensity-outlier: recAN individuals, day 1: 6.84 ± 6.87, day 2: 7.75 ± 6.23; HC, day 1: 5.27 ± 4.47, day 2: 8.14 ± 6.66).

On the single-subject level, a general linear model (GLM) was fit to model the hemodynamic response to increasing reward levels. We modeled all four reward levels of the anticipation, motor response and feedback phase as single events (12 regressors). Additional regressors included six motion parameters as well as one regressor for each motion or intensity outlier volume (see SM 6).

To test our hypothesis regarding the effect of ATD on reward processing in AN in comparison to HC with second-level whole-brain analyses, we used neuropointillist (http://ibic.github.io/neuropointillist/; Madhyastha et al., Reference Madhyastha, Peverill, Koh, McCabe, Flournoy, Mills and McLaughlin2018) to fit linear mixed models in R Studio (nlme package) to each voxel for each participant separately for the anticipation and feedback phase during both time points. The mixed model to investigate the three-way interaction of ATD, group and reward comprised the four centered reward levels, group as well as individual TRP/LNAA ratios as indicators of the ATD condition. This procedure then yields statistical parameter maps for each main and interaction effect. To control for false-positives, family-wise error (FWE) correction was performed using 3DClustSim (http://afni.nimh.nih.gov/afni; ‘fixed’ version compiled June 2017). Afterward, to aid interpretation of significant whole-brain results and since neuropointillist only yields statistical parameter maps, we obtained extracted beta values averaged from significant clusters of three-way interaction effects using the MarsBaR toolbox for SPM (Brett, Anton, Valabregue, & Poline, Reference Brett, Anton, Valabregue and Poline2002) and ran the same linear mixed models (in a post-hoc approach) with the extracted indices using R Studio (nlme package).