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Journal ArticleDOI

An obesity-associated risk allele within the FTO gene affects human brain activity for areas important for emotion, impulse control and reward in response to food images.

Lyle Wiemerslage1, Emil K. Nilsson1, Linda Solstrand Dahlberg1, Fia Ence-Eriksson1, Sandra Castillo1, Anna L. Larsen1, Simon B. A. Bylund1, Pleunie S. Hogenkamp1, Gaia Olivo1, Marcus Bandstein1, Olga E. Titova1, Elna-Marie Larsson1, Christian Benedict1, Samantha J. Brooks2, Helgi B. Schiöth1 
Uppsala University1, University of Cape Town2
21 Feb 2016-European Journal of Neuroscience (Wiley)-Vol. 43, Iss: 9, pp 1173-1180
TL;DR: The results suggest that the two genotypes are associated with differential neural processing of food images, which may influence weight status through diminished impulse control and reward processing.
Abstract: Understanding how genetics influences obesity, brain activity and eating behaviour will add important insight for developing strategies for weight-loss treatment, as obesity may stem from different causes and as individual feeding behaviour may depend on genetic differences. To this end, we examined how an obesity risk allele for the FTO gene affects brain activity in response to food images of different caloric content via functional magnetic resonance imaging (fMRI). Thirty participants homozygous for the rs9939609 single nucleotide polymorphism were shown images of low- or high-calorie food while brain activity was measured via fMRI. In a whole-brain analysis, we found that people with the FTO risk allele genotype (AA) had increased activity compared with the non-risk (TT) genotype in the posterior cingulate, cuneus, precuneus and putamen. Moreover, higher body mass index in the AA genotype was associated with reduced activity to food images in areas important for emotion (cingulate cortex), but also in areas important for impulse control (frontal gyri and lentiform nucleus). Lastly, we corroborate our findings with behavioural scales for the behavioural inhibition and activation systems. Our results suggest that the two genotypes are associated with differential neural processing of food images, which may influence weight status through diminished impulse control and reward processing.

Summary (4 min read)

Jump to: [INTRODUCTION][FTO Associated Brain Activity 5][Participants][Behavioral Questionnaires][Preprocessing of fMRI data][Statistical Analysis][RESULTS][Differential patterns of behavior for each FTO genotype depending on body-mass index.][DISCUSSION][FTO Associated Brain Activity 14] and [B)]

INTRODUCTION

  • Several different FTO single nucleotide polymorphisms (SNPs) are associated with a higher body mass index (BMI) (Sällman Almén et al., 2013; Scuteri et al., 2007a) , and higher energy intake (Speakman, 2013) .
  • Moreover, experiments in rodents show that changes in FTO expression levels in the hypothalamus affect feeding behavior (Frederiksen, Skakkebaek, & Andersson, 2007; Olszewski et al., 2009; Tung et al., 2010) .
  • Personality scales for the Behavioral Inhibition System (BIS) and Behavioral Activation System (BAS), which measure punishment and reward sensitivity respectively, are two such tools which correlate with inactivity and poor diet (Carver & White, 1994; Dietrich, Federbusch, Grellmann, Villringer, & Horstmann, 2014; Meule, 2013; Voigt et al., 2009) .

FTO Associated Brain Activity 5

  • To date, however, few fMRI studies have examined how genetic profile is associated with brain responses to food in obesity.
  • A recent study found that people with the FTO risk allele for rs8050136 had reduced activity in the right prefrontal cortex while viewing food images in a postprandial state, but not while fasting (Heni et al., 2014) .
  • Notably, their cohort of participants had a normal BMI with no obese participants.
  • Against this background, the authors explore for the first time the association between FTO genotype, BMI, and neural responses to food images of either low-or high-calorie content.

Participants

  • Prior to any experimental procedures, all participants gave written informed consent to the study which conformed to the Declaration of Helsinki and approved by the local ethics committee.
  • Genotyping of the FTO single nucleotide polymorphism (SNP) rs9939609 was performed with a pre-designed Taqman single-nucleotide polymorphism genotyping assay (Applied Biosystems, Foster City, USA) and an ABI7900 genetic analyzer with SDS 2.2 software at the Uppsala Genome Center (http://www.genpat.uu.se/node462).
  • Only homozygous participants were included in the study.
  • Hunger ratings were also assessed on a 1-10 scale with higher numbers indicating greater feelings of hunger.

Behavioral Questionnaires

  • Clinical measures for punishment sensitivity and reward-seeking behavior were acquired using the Behavioral Inhibition System (BIS) and Behavioral Activation System (BAS) questionnaires (Carver & White, 1994) .
  • Each item was represented by a statement, where the participant indicated how much s/he agreed or FTO Associated Brain Activity 7 disagreed on a four-point scale.
  • The BIS included only one scale, evaluating the reactions to the anticipation of punishment and anxiety, while the BAS included three subscales: Drive, which represents the pursuit of desired goals; Fun Seeking, which evaluates the desire for new rewards and impulsivity; and Reward Responsiveness, which focuses on positive reactions anticipating rewards.

Preprocessing of fMRI data

  • All preprocessing steps were performed using software package Statistical Parametric Mapping (SPM, version 8, http://www.fil.ion.ucl.ac.uk/spm/), implemented in MATLAB (version R2014a, 11 FEB 2014 .
  • The images were realigned and estimated to remove movement artefacts in the data.
  • EPI images were further matched with the structural image using coregistration.
  • The anatomical image was segmented to strip away unnecessary tissue in the images.
  • Tissue probability maps were introduced in the segmentation step to differentiate between gray matter, white matter and cerebrospinal fluid in each individual.

Statistical Analysis

  • All fMRI statistical analysis was performed using the same versions of SPM and MATLAB listed in preprocessing steps.
  • For all whole-brain results, a family wise error FTO Associated Brain Activity 9 (FWE) corrected significance level was set at p < 0.05 to correct for multiple testing.
  • This contrast was then tested using a between-groups t-test followed by directional post-hoc comparisons as well as with a multiple regression analysis testing for interactions between genotype and BMI, BIS, or BAS individually.
  • Bilateral masks of such areas were produced using the Wake Forest University Pickatlas toolbox (Maldjian, Laurienti, Kraft, & Burdette, 2003) within SPM.
  • Results for the PCA were considered significant if the percentage of inertia summing from the two largest eigenvalues exceeded values listed in a significance table based on 10,000 analyses with similar numbers of individuals and independent variables (Lê et al., 2008) .

RESULTS

  • The obesity-associated FTO SNP rs9939609, is associated with increased activity in response to food images.
  • BOLD signals were measured as participants were shown images of low-calorie (LC) food, high-calorie (HC) food, or control images in a block design format.
  • Areas included the posterior cingulate cortex (PCC), cingulate gyrus, cuneus, and precuneus (Table 2 ).
  • A multiple regression analysis found an interaction between genotype and BMI, post-hoc comparisons found significant clusters for the AA genotype while BMI was decreasing in the PCC, cingulate gyrus, middle occipital gyrus, and precuneus (Supplementary Table 1 ).
  • Within the t-test comparison between genotypes, a significant cluster showing greater activity in the AA genotype was FTO Associated Brain Activity 11 found in the putamen after performing a small-volumes correction using a 6 mmradius sphere over the lowest FWE-corrected p-value in the cluster (Table 2 ).

Differential patterns of behavior for each FTO genotype depending on body-mass index.

  • The authors next tested if behavioral questionaires corrobarated the findings from the imaging experiments.
  • The authors then performed a principle component analysis within each genotype using the BIS and the three BAS subscales (Drive, Fun Seeking, and Reward Responsiveness) as variables of interest with BMI as a quantitative supplementary variable.
  • For both analyses, all the variables of interest were well projected and the first two dimensions accounted for ≈80% of the variablity (considered significant based on critera listed in methods under statistical analysis subheading, 81.4 > 80.0 for the AA group and 79.2 > 76.5 in the TT group).
  • Moreover, the variables of interest projected to the same quandrants except for the Drive and Fun Seeking subscales, which were switched between the two different genotypes.
  • Furthermore, the authors followed up the association between the BIS and BMI using a multiple regression analysis testing if BIS scores could be predicted by genotype, BMI, or their interaction.

DISCUSSION

  • The authors examined whether an obesity-associated genotype affects the neural processing of food images with different caloric content and to what extent body-mass index (BMI) is an important factor.
  • The authors found the AA genotype had increased brain activity compared to the TT genotype when viewing food images with different caloric contents, specifically in areas important for emotion (cingulate gyrus), memory, and self-image (cuneus and precuneus) and reward .
  • Thus, discrimination between HC and LC foods may be handled differently for each genotype depending on BMI.
  • Next, the authors corroborate their findings in the imaging study with personality questionnaires examining behavioral characteristics related to impulsivity and rewardprocessing: namely the Behavioral Inhibition System (BIS) and Behavioral Activation System (BAS) scales.
  • The authors found that the BIS as well as subscales of the BAS correlated with BMI oppositely in each genotype.

FTO Associated Brain Activity 14

  • In between-groups comparisons, as well as multiple regression analysis, the authors found significant clusters of brain activity when testing a contrast for caloric discrimination (HC food images opposed to LC food images).
  • Specifically, the authors found increased neural activation in the AA genotype compared to the TT genotype within the posterior cingulate cortex (PCC), cingulate gyrus, cuneus and precuneus.
  • The PCC is a well-connected and multifunctional brain area associated with emotional processing, and a central node in the default mode network (DMN): involved in arousal/awareness, balancing external and internal thought, and emotion (Leech & Sharp, 2014) .
  • Thus, the AA genotype in their cohort confirms previous reports equating impulsivity with obesity/overeating (Meule, 2013) specifically in one study which also found a negative correlation between BIS and BMI in males (Dietrich et al., 2014) .
  • In conclusion, their findings offer insight into the relationship between FTO, obesity, and brain activity; and suggest that overweight/obese populations have different attitudes and functional processing for food images depending on genetic background.

B)

  • A region of interest analysis found a significant cluster within the putamen after a smallvolumes correction.
  • The BIS evaluates inhibitory behavior in the anticipation of punishment and anxiety, while the BAS included three subscales: Drive, which represents the pursuit of desired goals; Fun Seeking, which evaluates the desire for new rewards and impulsivity; and Reward Responsiveness, which focuses on positive reactions anticipating rewards.
  • The behavioral variables were all well projected in each group.
  • A) variables factor map for the AA genotype.
  • BMI was positively correlated with BIS and negatively correlated with the BAS Fun Seeking subscale.

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Wiemerslage, L, Nilsson, EK, Solstrand Dahlberg, L, Ence-Eriksson, F, Castillo,
S, Larsen, AL, Bylund, SBA, Hogenkamp, PS, Olivo, G, Bandstein, M, Titova,
OE, Larsson, E-M, Benedict, C, Brooks, SJ and Schiöth, HB
An obesity-associated risk allele within the FTO gene affects human brain
activity for areas important for emotion, impulse control and reward in
response to food images.
http://researchonline.ljmu.ac.uk/id/eprint/9287/
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Citation (please note it is advisable to refer to the publisher’s version if you
intend to cite from this work)
Wiemerslage, L, Nilsson, EK, Solstrand Dahlberg, L, Ence-Eriksson, F,
Castillo, S, Larsen, AL, Bylund, SBA, Hogenkamp, PS, Olivo, G, Bandstein,
M, Titova, OE, Larsson, E-M, Benedict, C, Brooks, SJ and Schiöth, HB (2016)
An obesity-associated risk allele within the FTO gene affects human brain
LJMU Research Online
http://researchonline.ljmu.ac.uk/
FTO Associated Brain Activity 1
Title 1
An obesity-associated risk allele within the FTO gene affects brain activity for areas 2
important for emotion, impulse control, and reward in response to food images. 3
4
Running Title 5
FTO Associated Brain Activity 6
7
Author names and affiliation 8
Lyle Wiemerslage*
§
, Emil K Nilsson
§
, Linda Solstrand Dahlberg
§
, Fia Ence-Eriksson
§
, 9
Sandra Castillo
§
, Anna L Larsen
§
, Simon BA Bylund
§
, Pleunie S Hogenkamp
§
, Gaia 10
Olivo
§
, Marcus Bandstein
§
, Olga E Titova
§
, Elna-Marie Larsson
, Christian Benedict
§
, 11
Samantha J Brooks
, Helgi B Schiöth
§
12
13
Uppsala University § 14
Department of Neuroscience, Functional Pharmacology 15
Biomedicinska Centrum (BMC) 16
Husargatan 3, Box 593 17
751 24 Uppsala, Sweden 18
19
Section of Neuroradiology 20
Department of Radiology, Uppsala University 21
Akademiska Sjukhuset 22
751 85 Uppsala, Sweden 23
24
University of Cape Town 25
Department of Psychiatry 26
Old Groote Schuur Hospital 27
J2 Building 28
Anzio Road 29
Observatory, Cape Town, South Africa. 30
31
Corresponding author 32
Uppsala University * 33
Department of Neuroscience, Functional Pharmacology 34
Biomedicinska Centrum (BMC) 35
FTO Associated Brain Activity 2
Husargatan 3, Box 593 36
751 24 Uppsala, Sweden 37
lyle.wiemerslage@neuro.uu.se 38
39
Number of: 40
Figures = 3 41
Tables = 1 42
Words: 43
o Abstract = 197 44
o Introduction = 565 45
o Entire Manuscript (excluding references and figure legends) = 3,972 46
47
Keywords: 48
FTO, fMRI, SNP, obesity, food 49
50
Conflict of Interest: 51
The authors declare no conflicts of interest. 52
FTO Associated Brain Activity 3
ABSTRACT 53
Understanding how genetics influences obesity, brain activity, and eating behavior will 54
add important insight for developing strategies for weight-loss treatment, as obesity may stem 55
from different causes and as individual feeding behavior may depend on genetic differences. 56
To this end, we examined how an obesity risk-allele for the FTO gene affects brain activity in 57
response to food images of different caloric content via fMRI. 30 participants homozygous 58
for the rs9939609 single nucleotide polymorphism were shown images of low- or high-calorie 59
food while brain activity was measured via fMRI. In a whole-brain analysis, we found that 60
people with the FTO risk-allele genotype (AA) had increased activity than the non-risk (TT) 61
genotype in the posterior cingulate, cuneus, precuneus, and putamen. Moreover, higher BMI 62
in the AA genotype was associated with reduced activity to food images in areas important for 63
emotion (cingulate cortex), but also in areas important for impulse control (frontal gyri and 64
lentiform nucleus). Lastly, we corroborate our findings with behavioral scales for the 65
behavioral inhibition and activation systems (BIS/BAS). Our results suggest that the two 66
genotypes are associated with differential neural processing of food images, which may 67
influence weight status through diminished impulse control and reward processing. 68
69
Keywords: 70
fMRI, FTO, SNP, BMI, food images, obesity 71
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References
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Journal ArticleDOI
Personality traits and obesity: a systematic review.

[...]

G. Gerlach1, Stephan Herpertz1, Sabine Loeber2, Sabine Loeber1
Ruhr University Bochum1, University of Bamberg2
01 Jan 2015-Obesity Reviews
TL;DR: The results of the present review suggest that, within the context of therapeutic weight reduction measures, it is meaningful to identify subgroups of patients for whom specific treatment options need to be developed, such as measures for strengthening self‐control skills.
Abstract: Based on a bio-social-ecological systems model of the development and maintenance of obesity, there has been in the last few years a growing research interest in the association of obesity and personality traits. The aim of the present review was a comprehensive and critical evaluation of the existing literature taking into account the methodological quality of studies to enhance our understanding of personality traits associated with body weight, the development of overweight and obesity as well as the effectiveness of weight loss interventions including bariatric surgery. Personality traits play an important role both as risk as well as protective factors in the development of overweight and obesity. While thus in particular 'neuroticism', 'impulsivity' and 'sensitivity to reward' appear as risk factors, 'conscientiousness' and 'self-control' have been shown to have a protective function in relation to weight gain. Conscientiousness is a measure of regulation of internal urges and self-discipline, and may thus provide a potential source of control over impulsive reward-oriented behaviour. The results of the present review suggest that, within the context of therapeutic weight reduction measures, it is meaningful to identify subgroups of patients for whom specific treatment options need to be developed, such as measures for strengthening self-control skills.

224 citations

"An obesity-associated risk allele w..." refers background in this paper

  • ...Indeed, obesity may depend on psychological characteristics, specifically those related to reward or selfcontrol (Gerlach et al., 2015)....

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Journal ArticleDOI
Hypothalamic-specific manipulation of Fto, the ortholog of the human obesity gene FTO, affects food intake in rats

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Yi Chun Loraine Tung1, Eduard Ayuso2, Xiaoye Shan1, Fatima Bosch2, Stephen O'Rahilly1, Anthony P. Coll1, Giles S.H. Yeo1 
University of Cambridge1, Autonomous University of Barcelona2
19 Jan 2010-PLOS ONE
TL;DR: It is demonstrated that consumption of a high fat diet results in a 2.5 fold increase in Arc Fto expression, the first indication that selective alteration of Fto levels in the hypothalamus can influence food intake, consistent with the reported effects of FTO alleles on appetite and food intake in man.
Abstract: Sequence variants in the first intron of FTO are strongly associated with human obesity and human carriers of the risk alleles show evidence for increased appetite and food intake. Mice globally lacking Fto display a complex phenotype characterised by both increased energy expenditure and increased food intake. The site of action of FTO on energy balance is unclear. Fasting reduces levels of Fto mRNA in the arcuate nucleus (ARC) of the hypothalamus, a site where Fto expression is particularly high. In this study, we have extended this nutritional link by demonstrating that consumption of a high fat diet (45%) results in a 2.5 fold increase in Arc Fto expression. We have further explored the role of hypothalamic Fto in the control of food intake by using stereotactic injections coupled with AAV technology to bi-directionally modulate Fto expression. An over expression of Fto protein by 2.5-fold in the ARC results in a 14% decrease in average daily food intake in the first week. In contrast, knocking down Arc Fto expression by 40% increases food intake by 16%. mRNA levels of Agrp, Pomc and Npy, ARC-expressed genes classically associated with the control of food intake, were not affected by the manipulation of Fto expression. However, over expression of Fto resulted in a 4-fold increase in the mRNA levels of Stat3, a signalling molecule critical for leptin receptor signalling, suggesting a possible candidate for the mediation of Fto's actions. These data provide further support for the notion that FTO itself can influence key components of energy balance, and is therefore a strong candidate for the mediation of the robust association between FTO intronic variants and adiposity. Importantly, this provide the first indication that selective alteration of FTO levels in the hypothalamus can influence food intake, a finding consistent with the reported effects of FTO alleles on appetite and food intake in man.

168 citations

Journal ArticleDOI
Carver and White's (1994) BIS/BAS scales and their relationship to risky health behaviours

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Danielle C. Voigt1, James Price Dillard1, Kurt Braddock1, Jason W. Anderson2, Pradeep Sopory3, Michael T. Stephenson4 
Pennsylvania State University1, Minnesota State University Moorhead2, Wayne State University3, Texas A&M University4
01 Jul 2009-Personality and Individual Differences
TL;DR: In this article, Carver and White's (1994) BIS and BAS subscales (Reward Responsiveness, Drive, and Fun Seeking) were tested against seven health composites including sex, alcohol, drug, and tobacco use, safety, inactivity, and poor diet.

137 citations

"An obesity-associated risk allele w..." refers result in this paper

  • ...…scales for the Behavioral Inhibition System (BIS) and Behavioral Activation System (BAS), which measure punishment and reward sensitivity, respectively, are two such tools which correlate with inactivity and poor diet (Carver & White, 1994; Voigt et al., 2009; Meule, 2013; Dietrich et al., 2014)....

    [...]

  • ...The correlation between the Drive subscale and BMI in the AA genotype corrobo- rates previous associations with BAS, arousal and overeating (Voigt et al., 2009) and also a previous fMRI report associating the Drive subscale with neural activity in response to appetitive food images (Beaver et al.,…...

    [...]

  • ...Lastly, we corroborate our findings in the imaging study with personality measures from the BIS and BAS scales, as obesity is associated with anomalies in both (Carver & White, 1994; Voigt et al., 2009; Meule, 2013; Dietrich et al., 2014)....

    [...]

Journal ArticleDOI
The cerebellum in feeding control: possible function and mechanism.

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Jing-Ning Zhu1, Jian-Jun Wang1
Nanjing University1
25 Feb 2008-Cellular and Molecular Neurobiology
TL;DR: It is described that the cerebellum may be much more than a movement coordinator and actively participate in feeding control, i.e., it may act as an essential node linking somatic and visceral systems and help to generate an integrated and coordinated somatic-visceral response in feeding behavior.
Abstract: Accumulating anatomical, functional, and behavioral studies reveal that the cerebellum is involved in the regulation of various visceral functions including feeding control. Cerebellar lesions may induce alterations in feeding behavior and decreases in body weight. Although the exact mechanisms underlying the cerebellar regulation of food intake is still unclear, a series of studies have demonstrated that there are neural pathways directly and/or indirectly connecting the cerebellum with several important centers for feeding control, such as the hypothalamus. Electrophysiological data suggest that via the direct cerebellohypothalamic projections, the cerebellar outputs may reach, converge, and be integrated with some critical feeding signals including gastric vagal afferents, CCK, leptin, and glycemia on single hypothalamic neurons. Furthermore, recent functional imaging studies provide substantial evidences that hunger, satiation, and thirst are accompanied with a cerebellar activation. Here we describe that the cerebellum may be much more than a movement coordinator and actively participate in feeding control, i.e., it may act as an essential node linking somatic and visceral systems and help to generate an integrated and coordinated somatic-visceral response in feeding behavior.

128 citations

Additional excerpts

  • ...Our findings of altered activity among AA participants in cerebellar areas are also pertinent, given the relatively recent association with the cerebellum to emotion (Schienle & Scharm€uller, 2013) and appetitive processes (Zhu & Wang, 2007)....

    [...]

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Relation of obesity to neural activation in response to food commercials

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Ashley N. Gearhardt1, Sonja Yokum1, Eric Stice1, Jennifer L. Harris1, Kelly D. Brownell1 
Oregon Research Institute1
01 Jul 2014-Social Cognitive and Affective Neuroscience
TL;DR: This study is the first to examine how neural response to food commercials differs from other stimuli and to explore how this response may differ by weight status and to inform current policy debates regarding the impact of food advertising to minors.
Abstract: Adolescents view thousands of food commercials annually, but the neural response to food advertising and its association with obesity is largely unknown. This study is the first to examine how neural response to food commercials differs from other stimuli (e.g. non-food commercials and television show) and to explore how this response may differ by weight status. The blood oxygen level-dependent functional magnetic resonance imaging activation was measured in 30 adolescents ranging from lean to obese in response to food and non-food commercials imbedded in a television show. Adolescents exhibited greater activation in regions implicated in visual processing (e.g. occipital gyrus), attention (e.g. parietal lobes), cognition (e.g. temporal gyrus and posterior cerebellar lobe), movement (e.g. anterior cerebellar cortex), somatosensory response (e.g. postcentral gyrus) and reward [e.g. orbitofrontal cortex and anterior cingulate cortex (ACC)] during food commercials. Obese participants exhibited less activation during food relative to non-food commercials in neural regions implicated in visual processing (e.g. cuneus), attention (e.g. posterior cerebellar lobe), reward (e.g. ventromedial prefrontal cortex and ACC) and salience detection (e.g. precuneus). Obese participants did exhibit greater activation in a region implicated in semantic control (e.g. medial temporal gyrus). These findings may inform current policy debates regarding the impact of food advertising to minors.

124 citations

"An obesity-associated risk allele w..." refers result in this paper

  • ...The cuneus and precuneus are also implicated in obesity, as a previous study showed that obese adolescents had less activation in the cuneus and precuneus when viewing food vs. non-food commercials (Gearhardt et al., 2014)....

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Q1. What are the contributions in this paper?

56 To this end, the authors examined how an obesity risk-allele for the FTO gene affects brain activity in 57 response to food images of different caloric content via fMRI. Their results suggest that the two 66 genotypes are associated with differential neural processing of food images, which may 67 influence weight status through diminished impulse control and reward processing.