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"apellidos" => "Carrascosa" ] ] ] ] "resumen" => array:1 [ 0 => array:3 [ "titulo" => "Graphical abstract" "clase" => "graphical" "resumen" => "<span id="abst0005" class="elsevierStyleSection elsevierViewall"><p id="spar0005" class="elsevierStyleSimplePara elsevierViewall"><elsevierMultimedia ident="fig0015"></elsevierMultimedia></p></span>" ] ] ] "idiomaDefecto" => "es" "EPUB" => "https://multimedia.elsevier.es/PublicationsMultimediaV1/item/epub/S0001731023005331?idApp=UINPBA000044" "url" => "/00017310/0000011500000001/v1_202401030514/S0001731023005331/v1_202401030514/es/main.assets" ] ] "en" => array:20 [ "idiomaDefecto" => true "cabecera" => "<span class="elsevierStyleTextfn">Review</span>" "titulo" => " Glucagon-Like Peptide-1 Agonists for Treating Obesity in Patients With Immune-Mediated Skin Diseases" "tieneTextoCompleto" => true "paginas" => array:1 [ 0 => array:2 [ "paginaInicial" => "T56" "paginaFinal" => "T65" ] ] "autores" => array:1 [ 0 => array:4 [ "autoresLista" => "E. 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"apellidos" => "Carrascosa" "referencia" => array:1 [ 0 => array:2 [ "etiqueta" => "<span class="elsevierStyleSup">g</span>" "identificador" => "aff0035" ] ] ] ] "afiliaciones" => array:7 [ 0 => array:3 [ "entidad" => "Servicio de Dermatología, Hospital de la Santa Creu i Sant Pau, Barcelona, Spain" "etiqueta" => "a" "identificador" => "aff0005" ] 1 => array:3 [ "entidad" => "Servicio de Endocrinología y Nutrición, Hospital Universitario Son Llàtzer, Instituto de Investigación Sanitaria Illes Balears (IdISBa), Clínica Rotger (Grupo Quirón), Palma de Mallorca, Baleares, Spain" "etiqueta" => "b" "identificador" => "aff0010" ] 2 => array:3 [ "entidad" => "Servicio de Dermatología, Hospital Universitario Infanta Leonor, Comunidad de Madrid, Spain" "etiqueta" => "c" "identificador" => "aff0015" ] 3 => array:3 [ "entidad" => "Departamento de Medicina, Universitat Autònoma de Barcelona, Barcelona; Servicio de Endocrinología y Nutrición, Hospital del Mar, IMIM Institut Mar d’Investigacions Mediques, Parc de Salut Mar, Barcelona; CIBEROBN, Instituto de Salud Carlos III (ISCIII), Madrid, Spain" "etiqueta" => "d" "identificador" => "aff0020" ] 4 => array:3 [ "entidad" => "Servicio de Dermatología, Hospital del Mar, Parc de Salut Mar, Barcelona, Spain" "etiqueta" => "e" "identificador" => "aff0025" ] 5 => array:3 [ "entidad" => "Servicio de Dermatología y Venereología, Hospital de Manises, Valencia, Spain" "etiqueta" => "f" "identificador" => "aff0030" ] 6 => array:3 [ "entidad" => "Servicio de Dermatología, Hospital Universitari Germans Trias i Pujol, Badalona, Spain" "etiqueta" => "g" "identificador" => "aff0035" ] ] "correspondencia" => array:1 [ 0 => array:3 [ "identificador" => "cor0005" "etiqueta" => "⁎" "correspondencia" => "Corresponding author." ] ] ] ] "titulosAlternativos" => array:1 [ "es" => array:1 [ "titulo" => "Agonistas del receptor de GLP-1 para el tratamiento de la obesidad en pacientes con dermatosis inmunomediadas" ] ] "resumenGrafico" => array:2 [ "original" => 1 "multimedia" => array:5 [ "identificador" => "fig0015" "tipo" => "MULTIMEDIAFIGURA" "mostrarFloat" => false "mostrarDisplay" => true "figura" => array:1 [ 0 => array:4 [ "imagen" => "fx1.jpeg" "Alto" => 1085 "Ancho" => 753 "Tamanyo" => 71948 ] ] ] ] "textoCompleto" => "<span class="elsevierStyleSections"><p id="par0005" class="elsevierStylePara elsevierViewall">Obesity is a common comorbidity in chronic inflammatory conditions such as psoriasis (PsO) and hidradenitis suppurativa (HS), in which the common underlying pathogenic mechanisms are closely related to those found in obesity. It will be interesting to see whether the new and effective therapeutic alternatives under development for obesity enable a more effective decrease in body weight, which, in turn, could be beneficial for the outcome of immune-mediated dermatoses.</p><span id="sec0005" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0030">Low-grade chronic inflammation and immunological imbalance facilitate a bidirectional association between obesity and immune-mediated dermatoses</span><p id="par0010" class="elsevierStylePara elsevierViewall">An excess of dysfunctional adiposity contributes to the inflammatory state that characterizes patients with obesity.<a class="elsevierStyleCrossRefs" href="#bib0440"><span class="elsevierStyleSup">1–4</span></a> As low-grade inflammation underlies obesity, PsO, and HS (<a class="elsevierStyleCrossRef" href="#sec0130">Fig. S1 of additional material</a>), any intervention that dampens the mechanisms that lead to this state will be positive for any of the 3 conditions.<a class="elsevierStyleCrossRefs" href="#bib0460"><span class="elsevierStyleSup">5,6</span></a> The mechanisms that underlie the bidirectional association between obesity and immune-mediated diseases<a class="elsevierStyleCrossRef" href="#bib0470"><span class="elsevierStyleSup">7</span></a> have not been clearly established, although it is accepted that the skin plays a causative role in chronic inflammation and immune disorders (<a class="elsevierStyleCrossRef" href="#sec0130">Fig. S2 additional material</a>).<a class="elsevierStyleCrossRefs" href="#bib0470"><span class="elsevierStyleSup">7,8</span></a></p><p id="par0015" class="elsevierStylePara elsevierViewall">The incidence of PsO and HS has increased in western countries in recent decades.<a class="elsevierStyleCrossRefs" href="#bib0480"><span class="elsevierStyleSup">9,10</span></a> Obesity has increased in parallel, and could be responsible, at least partially, for the aforementioned increase.<a class="elsevierStyleCrossRef" href="#bib0475"><span class="elsevierStyleSup">8</span></a></p><span id="sec0010" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0035">Psoriasis and obesity</span><p id="par0020" class="elsevierStylePara elsevierViewall">The prevalence of obesity is higher among patients with PsO than in the general population.<a class="elsevierStyleCrossRefs" href="#bib0490"><span class="elsevierStyleSup">11–18</span></a> In addition, obesity increases the risk of PsO,<a class="elsevierStyleCrossRefs" href="#bib0465"><span class="elsevierStyleSup">6,19,20</span></a> the incidence of which could be twice as great in patients with grade II/III obesity compared with subjects with normal weight.<a class="elsevierStyleCrossRef" href="#bib0540"><span class="elsevierStyleSup">21</span></a> Among the molecular mediators at the intersection between the 2 conditions are 3 adipokines—leptin, resistin, and adiponectin—whose levels impact the severity of PsO in patients with obesity.<a class="elsevierStyleCrossRefs" href="#bib0545"><span class="elsevierStyleSup">22–24</span></a></p><p id="par0025" class="elsevierStylePara elsevierViewall">Many complications associated with obesity are also associated with PsO. There is a higher prevalence of type 2 diabetes mellitus (DT2) in patients with PsO than in the general population.<a class="elsevierStyleCrossRef" href="#bib0560"><span class="elsevierStyleSup">25</span></a> In addition, insulin resistance induces dyslipidemia and contributes to the development of nonalcoholic hepatic steatosis (NAHS).<a class="elsevierStyleCrossRef" href="#bib0565"><span class="elsevierStyleSup">26</span></a> Cardiovascular risk (CVR) is increased in patients with obesity and PsO who present psoriatic arthritis, and who often have other risk factors.<a class="elsevierStyleCrossRef" href="#bib0570"><span class="elsevierStyleSup">27</span></a> The guidelines for the European Cardiology Society state that the body mass index (BMI) should not exceed 25<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>,<a class="elsevierStyleCrossRef" href="#bib0575"><span class="elsevierStyleSup">28</span></a> and so early interventions to manage obesity or excess weight associated with PsO could contribute to preventing CVR. Finally, obesity is associated with worse response to drugs for PsO (<a class="elsevierStyleCrossRef" href="#sec0130">Table S1 additional material</a>).<a class="elsevierStyleCrossRefs" href="#bib0580"><span class="elsevierStyleSup">29,30</span></a></p></span><span id="sec0015" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0040">Hidradenitis suppurativa and obesity</span><p id="par0030" class="elsevierStylePara elsevierViewall">There is a higher prevalence of obesity in subjects with HS than in the general population,<a class="elsevierStyleCrossRefs" href="#bib0590"><span class="elsevierStyleSup">31,32</span></a> and HS is detected more frequently in children with obesity.<a class="elsevierStyleCrossRef" href="#bib0600"><span class="elsevierStyleSup">33</span></a> The association between HS and obesity, as is the case for PsO, is also bidirectional, with low-grade inflammation as the unifying thread. Inflammatory imbalance in obesity perpetuates inflammation and follicular occlusion. Multiple molecular mechanisms, activated by inflammatory mediators, contribute to the progression of HS.<a class="elsevierStyleCrossRefs" href="#bib0605"><span class="elsevierStyleSup">34,35</span></a></p><p id="par0035" class="elsevierStylePara elsevierViewall">The prevalence of DT2 is higher in subjects with HS than in the general population.<a class="elsevierStyleCrossRef" href="#bib0615"><span class="elsevierStyleSup">36</span></a> HS is also associated with other conditions traditionally linked with obesity, such as metabolic syndrome, polycystic ovarian syndrome, and inflammatory bowel disease,<a class="elsevierStyleCrossRefs" href="#bib0620"><span class="elsevierStyleSup">37–39</span></a> and patients with HS are exposed to higher CVR than the general population.<a class="elsevierStyleCrossRef" href="#bib0635"><span class="elsevierStyleSup">40</span></a> Obesity negatively impacts the response of patients to the main treatments for HS (<a class="elsevierStyleCrossRef" href="#sec0130">Table S1 additional information</a>).<a class="elsevierStyleCrossRef" href="#bib0510"><span class="elsevierStyleSup">15</span></a></p></span></span><span id="sec0020" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0045">Advantages associated with weight loss in patients with obesity and psoriasis or hidradenitis suppurativa</span><p id="par0040" class="elsevierStylePara elsevierViewall">In addition to better response to treatments for inflammatory dermatoses, other arguments justify the desirability of patients with obesity and PsO or HS to lose weight.<ul class="elsevierStyleList" id="lis0005"><li class="elsevierStyleListItem" id="lsti0005"><span class="elsevierStyleLabel">•</span><p id="par0045" class="elsevierStylePara elsevierViewall">Weight loss is associated with a decrease in PsO severity and improved quality of life (QoL).<a class="elsevierStyleCrossRefs" href="#bib0640"><span class="elsevierStyleSup">41,42</span></a></p></li><li class="elsevierStyleListItem" id="lsti0010"><span class="elsevierStyleLabel">•</span><p id="par0050" class="elsevierStylePara elsevierViewall">Weight loss greater than 5% is associated with a higher rate of minimum disease activity in patients who are obese or overweight and in treatment for PsO.<a class="elsevierStyleCrossRefs" href="#bib0650"><span class="elsevierStyleSup">43,44</span></a></p></li><li class="elsevierStyleListItem" id="lsti0015"><span class="elsevierStyleLabel">•</span><p id="par0055" class="elsevierStylePara elsevierViewall">The Mediterranean diet, which facilitates weight loss, reduces psoriatic lesions.<a class="elsevierStyleCrossRef" href="#bib0660"><span class="elsevierStyleSup">45</span></a></p></li><li class="elsevierStyleListItem" id="lsti0020"><span class="elsevierStyleLabel">•</span><p id="par0060" class="elsevierStylePara elsevierViewall">Weight loss in patients with HS leads to a notable decrease in the number of lesions and, in some cases, disease remission.<a class="elsevierStyleCrossRef" href="#bib0665"><span class="elsevierStyleSup">46</span></a></p></li><li class="elsevierStyleListItem" id="lsti0025"><span class="elsevierStyleLabel">•</span><p id="par0065" class="elsevierStylePara elsevierViewall">Dysfunctional adiposity has been associated with worse indices of CVR and Dermatology Quality of Life Index (DLQI) in patients with HS.<a class="elsevierStyleCrossRef" href="#bib0670"><span class="elsevierStyleSup">47</span></a></p></li><li class="elsevierStyleListItem" id="lsti0030"><span class="elsevierStyleLabel">•</span><p id="par0070" class="elsevierStylePara elsevierViewall">The decrease in fatty tissue is associated with a decrease in molecular mechanisms that characterize the systemic inflammatory state.<a class="elsevierStyleCrossRef" href="#bib0675"><span class="elsevierStyleSup">48</span></a></p></li></ul></p></span><span id="sec0025" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0050">Specific treatments for weight loss</span><span id="sec0030" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0055">Diet and exercise</span><p id="par0075" class="elsevierStylePara elsevierViewall">Diet and exercise are the first therapeutic step but these interventions are, however, often insufficient to achieve favorable outcomes in skin diseases, good response to treatment for these conditions, and a decrease in CVR. Another limitation is the poor adherence and high drop-out rates.<a class="elsevierStyleCrossRef" href="#bib0680"><span class="elsevierStyleSup">49</span></a> Therefore, pharmacological options should also be explored. The limited number of treatments able to significantly reduce weight, as well as the risk of renewed weight gain from 6 months after the end of intervention, have been an obstacle for considering pharmacological treatment for obesity in patients with PsO or HS.<a class="elsevierStyleCrossRef" href="#bib0510"><span class="elsevierStyleSup">15</span></a></p></span><span id="sec0035" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0060">Approved and marketed drugs in Spain</span><span id="sec0040" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0065">Orlistat</span><p id="par0080" class="elsevierStylePara elsevierViewall">Orlistat is an inhibitor of the gastric and pancreatic lipases that block hydrolysis of triacyl glycerides and absorption of fatty acids through the intestinal endothelium. The drug is often associated with gastrointestinal adverse events, thereby hindering adherence. Its effect is modest, with weight losses of not more than 3% after 12 months, after which time, the weight is partially regained, even with continuing therapy.<a class="elsevierStyleCrossRef" href="#bib0685"><span class="elsevierStyleSup">50</span></a> There are no studies that have analyzed the effect of orlistat in patients with obesity and PsO or HS.</p></span><span id="sec0045" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0070">GLP-1 receptor agonists</span><p id="par0085" class="elsevierStylePara elsevierViewall">GLP-1 receptor agonists have recently made a mark as a possible pharmacological alternative for weight loss.</p></span><span id="sec0050" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0075">Indications, pleiotropic actions</span><p id="par0090" class="elsevierStylePara elsevierViewall">GLP-1 receptor agonists are analogs of GLP-1, an intestinal peptide hormone of ∼3.3 kDa belonging to the incretin family. On binding to the GLP-1 cell receptor, these agents trigger the same molecular mechanisms as those induced by the endogenous peptide. The interaction occurs in different tissues (pancreas, brain, myocardium, endothelium, kidney, digestive system), which means that its actions, including glycemic control with minimum risk of hypoglycemia, have a pleiotropic character (<a class="elsevierStyleCrossRef" href="#fig0005">Fig. 1</a>).<a class="elsevierStyleCrossRef" href="#bib0690"><span class="elsevierStyleSup">51</span></a> Moreover, a series of clinical trials suggest that the GLP-1 receptor agonists could induce cardiovascular protection.<a class="elsevierStyleCrossRefs" href="#bib0695"><span class="elsevierStyleSup">52–55</span></a></p><elsevierMultimedia ident="fig0005"></elsevierMultimedia></span><span id="sec0055" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0080">GLP-1 receptor agonists in the obesity setting</span><p id="par0095" class="elsevierStylePara elsevierViewall">The GLP-1 receptor agonists currently on the market have a molecule weight (MW) less than 5 kDa (except for dulaglutide), and a circulating half-life greater than the 5<span class="elsevierStyleHsp" style=""></span>minutes of the native GLP-1 molecule.<a class="elsevierStyleCrossRef" href="#bib0715"><span class="elsevierStyleSup">56</span></a> Brain nuclei such as the paraventricular nucleus of the thalamus and arcuate nucleus express GLP-1 receptors, although it is the former that appears to play the most important part in control of food intake.<a class="elsevierStyleCrossRefs" href="#bib0720"><span class="elsevierStyleSup">57,58</span></a> The GLP-1 receptor agonists for treatment of obesity in the European Union (EU), liraglutide (3<span class="elsevierStyleHsp" style=""></span>mg/day, subcutaneous) and semaglutide (2.4<span class="elsevierStyleHsp" style=""></span>mg in a weekly subcutaneous dose), are ><span class="elsevierStyleHsp" style=""></span>90% homologous with the structure of human GLP-1. Liraglutide has a half-life of 13<span class="elsevierStyleHsp" style=""></span>h, and reaches brain tissue on crossing the blood brain barrier. It is debated whether this action occurs by passive diffusion or, in contrast, requires interaction with the GLP-1 receptor.<a class="elsevierStyleCrossRefs" href="#bib0730"><span class="elsevierStyleSup">59–70</span></a> The semaglutide molecule has a longer aliphatic chain, conferring greater hydrophobicity. The incorporation of polyethylene glycol not only modifies its hydrolysis target by dipeptidyl peptidase-4, but also increases its affinity for albumin. These characteristics prolong its circulating half-life to up to 165<span class="elsevierStyleHsp" style=""></span>h, and, when conjugated with albumin, the molecule is able to penetrate the spinal chord, septal nucleus, and hypothalamus via the circumventricular organs.<a class="elsevierStyleCrossRef" href="#bib0735"><span class="elsevierStyleSup">60</span></a> Once in the satiety centers, liraglutide and semaglutide act on the neuronal populations of the pro-opiomelanocortin and NPY/AgRP neurons, implicated in metabolic activity, and, through as yet little known mechanisms, are able to reduce the hunger sensation. This action makes these agents a therapeutic option for weight loss.<a class="elsevierStyleCrossRef" href="#bib0715"><span class="elsevierStyleSup">56</span></a> Although to a lesser extent, delay in gastric emptying contributes to the anorexigenic effect.<a class="elsevierStyleCrossRef" href="#bib0740"><span class="elsevierStyleSup">61</span></a></p><p id="par0100" class="elsevierStylePara elsevierViewall">Clinical trials conducted with GLP-1 receptor agonists in patients with obesity (or excess weight [BMI ≥ 27] with comorbidities), or with DT2 and excess weight or obesity, have achieved weight reductions greater than those reported for orlistat, as well as those observed with oral antidiabetic agents such as the sodium glucose type 2 cotransporter inhibitors (SGLT2i) or metformin.<a class="elsevierStyleCrossRef" href="#bib0745"><span class="elsevierStyleSup">62</span></a> In a meta-analysis of more than 10 000 patients with obesity, those treated with GLP-1 receptor agonists lost, on average, 7<span class="elsevierStyleHsp" style=""></span>kg more than those in the control group.<a class="elsevierStyleCrossRef" href="#bib0750"><span class="elsevierStyleSup">63</span></a> Weight loss of up to 15% has been observed after 12 months of treatment,<a class="elsevierStyleCrossRefs" href="#bib0755"><span class="elsevierStyleSup">64,65</span></a> a level that had only been achieved through surgical methods.</p></span><span id="sec0060" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0085">Dosing, safety profile</span><p id="par0105" class="elsevierStylePara elsevierViewall">GLP-1 receptor antagonists with an indication for obesity (or excess weight [BMI ≥ 27<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>] with complications) are administered subcutaneously every week or daily. The use of GLP-1 receptor agonists is frequently associated with gastrointestinal adverse effects, particularly nausea, vomiting, diarrhea or constipation; these are transient and of mild to moderate intensity. Their onset can be avoided or the severity reduced to a large extent if dose escalation is performed as indicated in the label, and if, while treatment lasts, a series of well-defined dietary and behavioral recommendations are followed.<a class="elsevierStyleCrossRef" href="#bib0765"><span class="elsevierStyleSup">66</span></a> In patients who observe these recommendations, the adverse effects may disappear in a few days or weeks.<a class="elsevierStyleCrossRef" href="#bib0770"><span class="elsevierStyleSup">67</span></a></p></span><span id="sec0065" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0090">Arguments in favor of GLP-1 receptor agonists for weight control in patients with obesity and inflammatory dermatoses</span><p id="par0110" class="elsevierStylePara elsevierViewall">As mentioned earlier, weight loss has a positive effect on the outcome and response to treatments for PsO and HS. It is plausible to speculate that GLP-1 receptor agonists can induce greater weight loss than those obtained with other therapeutic interventions. This can also improve adherence. Furthermore, GLP-1 receptor agonists induce anti-inflammatory effects that could attenuate the low-grade inflammation that underlies obesity, PsO, and HS (reviewed recently in the context of PsO and psoriatic arthritis).<a class="elsevierStyleCrossRef" href="#bib0775"><span class="elsevierStyleSup">68</span></a> Finally, improved metabolic control and cardio-renal protection could be beneficial for reducing CVR and managing comorbidities such as DT2 or metabolic syndrome.</p></span><span id="sec0070" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0095">GLP-1 receptor agonists with indication for obesity</span><p id="par0115" class="elsevierStylePara elsevierViewall">As mentioned earlier, there are 2 GLT-1 receptor agonists indicated for the treatment of obesity in the EU in subjects with BMI ≥ 30<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span> or BMI ≥ 27<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span> and at least one weight-related comorbidity, always in combination with appropriate diet and physical exercise: liraglutide 3<span class="elsevierStyleHsp" style=""></span>mg and semaglutide 2.4 mg. The second, although approved by European Medicines Agency (EMA) and the Spanish Agency for Medicines and Health Products (AEMPS), is still not marketed in Spain.</p></span><span id="sec0075" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0100">Liraglutide 3<span class="elsevierStyleHsp" style=""></span>mg</span><p id="par0120" class="elsevierStylePara elsevierViewall">This agent is administered subcutaneously every day. The SCALE clinical trials were designed to assess the effectiveness and safety of this agent for weight loss in patients with obesity or overweight (BMI ≥ 27<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>) with comorbidities. <a class="elsevierStyleCrossRef" href="#tbl0005">Table 1</a> shows the most relevant findings. In a cohort of 3731 patients, weight loss of 5%, 10%, and 15% was observed in 63%, 33%, and 14%, respectively, after 56 weeks of treatment (27%, 11%, and 4% with placebo),<a class="elsevierStyleCrossRef" href="#bib0780"><span class="elsevierStyleSup">69</span></a> or of an additional 6% at 56 weeks in patients who had already lost 6% through hypocaloric diet and exercise.<a class="elsevierStyleCrossRef" href="#bib0785"><span class="elsevierStyleSup">70</span></a> Positive results were also observed in adolescent patients with obesity,<a class="elsevierStyleCrossRef" href="#bib0790"><span class="elsevierStyleSup">71</span></a> and in real-life studies substantial weight loss has also been reported.<a class="elsevierStyleCrossRefs" href="#bib0795"><span class="elsevierStyleSup">72–75</span></a></p><elsevierMultimedia ident="tbl0005"></elsevierMultimedia></span><span id="sec0080" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0105">Semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg</span><p id="par0125" class="elsevierStylePara elsevierViewall">In the STEP trials (<a class="elsevierStyleCrossRef" href="#tbl0005">Table 1</a>), designed to evaluate the efficacy and safety of semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg (subcutaneous, weekly) in patients with obesity, or excess weight (BMI ≥ 27<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>) with complications, weight loss of between 15% and 17% was achieved 68 weeks after starting treatment.<a class="elsevierStyleCrossRefs" href="#bib0815"><span class="elsevierStyleSup">76–78</span></a> In one of the trials, weight loss of 10% was reported after 20 weeks of therapy. The subjects who, at that time, switched from semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg to placebo had regained half of that weight after 48 weeks, whereas those who continued on active treatment achieved an additional weight loss of around 8% in the same time period. After 68 weeks with semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg, losses of 5%, 10%, and 15% were reported in 88%, 79%, and 63% of patients, respectively.<a class="elsevierStyleCrossRef" href="#bib0815"><span class="elsevierStyleSup">76</span></a> A recent meta-analysis concluded that semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg and liraglutide 3<span class="elsevierStyleHsp" style=""></span>mg are more efficacious than naltrexone-bupropion (not marketed in Spain) and orlistat.<a class="elsevierStyleCrossRef" href="#bib0830"><span class="elsevierStyleSup">79</span></a></p></span><span id="sec0085" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0110">Experience with liraglutide and semaglutide in psoriasis and hidradenitis suppurativa</span><span id="sec0090" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0115">Liraglutide and psoriasis</span><p id="par0130" class="elsevierStylePara elsevierViewall">In studies with liraglutide, patients with PsO and obesity had a diagnosis of DT2. and so the doses did not exceed 1.8<span class="elsevierStyleHsp" style=""></span>mg, which is the indicated dose for such patients. Although the series had limited sample sizes, the findings are interesting. In a cohort of 7 patients with DT2 and obesity, daily use of liraglutide 1.2<span class="elsevierStyleHsp" style=""></span>mg achieved, after 10 weeks, a weight reduction of 5% and a decrease in BMI of 2<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>.<a class="elsevierStyleCrossRef" href="#bib0835"><span class="elsevierStyleSup">80</span></a> In another study, 3 patients with DT2 and obesity achieved a decrease in BMI of between 0.8 and 3.8<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span> after 18 weeks with this same dose of liraglutide.<a class="elsevierStyleCrossRef" href="#bib0840"><span class="elsevierStyleSup">81</span></a> Another 2 patients with obesity and DT2 achieved weight losses of more than 5<span class="elsevierStyleHsp" style=""></span>kg and a decrease in BMI of 1.5 and 2<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span> after 6 weeks of treatment.<a class="elsevierStyleCrossRef" href="#bib0845"><span class="elsevierStyleSup">82</span></a> Finally, in a series of 20 subjects with obesity and DT2, an average weight loss of 4.7<span class="elsevierStyleHsp" style=""></span>kg was reported after 8 weeks of treatment with liraglutide 1.8<span class="elsevierStyleHsp" style=""></span>mg.<a class="elsevierStyleCrossRef" href="#bib0850"><span class="elsevierStyleSup">83</span></a> In most of these patients, improvements in the psoriasis area severity index (PASI) was observed, and on occasions, a decrease in psoriatic plaques. This observation could encourage investigation into whether this treatment is able to induce additional benefit.</p></span></span><span id="sec0095" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0120">Semaglutide and psoriasis</span><p id="par0135" class="elsevierStylePara elsevierViewall">Experience in this case is limited, and no studies have been performed with the 2.4<span class="elsevierStyleHsp" style=""></span>mg dose. There is a case report of a 73-year-old man with PsO, obesity, and DT2 who achieved a decrease in BMI from 40.3 to 38.3<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span> after 10 months treatment with 1<span class="elsevierStyleHsp" style=""></span>mg weekly of semaglutide.<a class="elsevierStyleCrossRef" href="#bib0855"><span class="elsevierStyleSup">84</span></a></p></span><span id="sec0100" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0125">Liraglutide and hidradenitis suppurativa</span><p id="par0140" class="elsevierStylePara elsevierViewall">Experience with this agent is limited in HS. There is a case report of a patient aged 19 years with HS and grade 2 obesity who started combination therapy with liraglutide 1.8<span class="elsevierStyleHsp" style=""></span>mg, metformin, levonorgestrel/ethinylestradiol, dapsone, and finasteride. She lost 16<span class="elsevierStyleHsp" style=""></span>kg in the first 6 months, although she then progressively regained weight.<a class="elsevierStyleCrossRef" href="#bib0860"><span class="elsevierStyleSup">85</span></a> There have been no reports of treatment of obesity with semaglutide in patients with HS.</p></span><span id="sec0105" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0130">Possibilities for use of GLP-1 receptor agonists in Spain for treatment of obesity</span><p id="par0145" class="elsevierStylePara elsevierViewall"><a class="elsevierStyleCrossRef" href="#fig0010">Figure 2</a> shows a schematic overview of the treatment options which are currently available for weight control in Spain and which are applicable to patients who also have PsO or HS. The doses of liraglutide or semaglutide are different depending on whether the patient has DT2, is overweight (BMI ≥ 27<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>) with comorbidities or has obesity (with or without DT2). In addition, in patients with DT2, there is the possibility of using an oral presentation of semaglutide. The effects of this presentation on weight and glycemia in clinical trials and real-world settings are comparable to those induced by the subcutaneous presentation, although a specific indication for weight control without DT2 is still lacking.<a class="elsevierStyleCrossRef" href="#bib0865"><span class="elsevierStyleSup">86</span></a> In order to avoid confusion in daily clinical practice, it is important to note that liraglutide 3<span class="elsevierStyleHsp" style=""></span>mg and semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg can be used in patients with DT2, provided these are obese or overweight with comorbidities. Patients with DT2 without obesity or excess weight with comorbidities can use liraglutide 1.8<span class="elsevierStyleHsp" style=""></span>mg (daily, subcutaneous) and semaglutide 1<span class="elsevierStyleHsp" style=""></span>mg (weekly, subcutaneous), or 14<span class="elsevierStyleHsp" style=""></span>mg (daily, oral) for glycemic control. However, they should not be treated with liraglutide 3<span class="elsevierStyleHsp" style=""></span>mg or semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg, because these doses are not indicated for this condition. The underlying reason is that, in the case of parenteral presentations, the effective doses of GLT-1 receptor agonists necessary for weight control are greater than those needed for glycemic control.</p><elsevierMultimedia ident="fig0010"></elsevierMultimedia></span><span id="sec0110" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0135">Other medium-term therapeutic options</span><p id="par0150" class="elsevierStylePara elsevierViewall">Tirzepatide, still not approved in the EU for specific use in patients with obesity, is a dual agonist of the GLP-1 receptors and another incretin, gastric inhibitor polypeptide (GIP). In a phase 3 trial in subjects with obesity or overweight (BMI ≥ 27<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>), its use for 18 months achieved weight loss of up to 20.9%.<a class="elsevierStyleCrossRef" href="#bib0870"><span class="elsevierStyleSup">87</span></a></p></span></span></span><span id="sec0115" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0140">Conclusions</span><p id="par0155" class="elsevierStylePara elsevierViewall"><ul class="elsevierStyleList" id="lis0010"><li class="elsevierStyleListItem" id="lsti0035"><span class="elsevierStyleLabel">•</span><p id="par0160" class="elsevierStylePara elsevierViewall">Low-grade inflammation underlies obesity and PsO/HS, and this inflammation has a negative impact on both conditions.</p></li><li class="elsevierStyleListItem" id="lsti0040"><span class="elsevierStyleLabel">•</span><p id="par0165" class="elsevierStylePara elsevierViewall">Weight loss is beneficial for PsO and HS outcomes, through a reduction in the inflammatory component of CVR.</p></li><li class="elsevierStyleListItem" id="lsti0045"><span class="elsevierStyleLabel">•</span><p id="par0170" class="elsevierStylePara elsevierViewall">GLP-1 receptor agonists, by achieving greater weight loss than obtained with other medications, may represent a therapeutic opportunity for improving obesity in patients with PsO and HS, with resulting decrease in CVR and, in general, improvement in the medium to long term.</p></li><li class="elsevierStyleListItem" id="lsti0050"><span class="elsevierStyleLabel">•</span><p id="par0175" class="elsevierStylePara elsevierViewall">The formation of multidisciplinary teams comprised of dermatologists and endocrinologists may contribute to better management of patients with obesity/overweight and immune-mediated dermatosis.</p></li></ul></p></span><span id="sec0120" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0145">Funding</span><p id="par0180" class="elsevierStylePara elsevierViewall">Laboratorios Novonordisk collaborated through funding for Medical Writing Services.</p></span><span id="sec0125" class="elsevierStyleSection elsevierViewall"><span class="elsevierStyleSectionTitle" id="sect0150">Conflicts of Interest</span><p id="par0185" class="elsevierStylePara elsevierViewall">Eva Vilarrasa has received fees for consulting and/or as a speader and/or for travel and/or has participated in clinical trials sponsored by Abbvie, Almirall, Amgen, Boehringer Ingelheim, Bristol-Meyers Squibb, Celgene, Gebro, Isdin, Janssen, LEO Pharma, Lilly, Merck Serono, MSD, Novartis, Pfizer, Roche, Sandoz, Sanofi, and UCB.</p><p id="par0190" class="elsevierStylePara elsevierViewall">Joana Nicolau has received fees for presentations and consulting on behalf of Sanofi, Novo Nordisk, Lilly, Boehringer-Ingelheim, Fresenius, AstraZeneca, Fresenius, Dexcom, Amgen, and Senseonics.</p><p id="par0195" class="elsevierStylePara elsevierViewall">Pablo de la Cueva has participated as consultant and/or investigator and/or speaker for the following pharmaceutical companies: Abbvie, Almirall, BMS, Boehringer-Ingelheim, Celgene, Janssen Cilag, LEO Pharma, Lilly, MSD, Novartis, Novo Nordisk, Pfizer, Roche, Sanofi, and UCB.</p><p id="par0200" class="elsevierStylePara elsevierViewall">Albert Goday has received fees for investigation projects, consulting, and postgraduate training, and has participated in clinical trials sponsored by Almirall, Ascensia, Colegio de Farmacéuticos de Barcelona, Esteve, Federación Farmacéutica, Fundación Catalana Síndrome de Down, Fundació Gol i Gorina, Instituto de Salud Carlos III, Jansen, Lilly, Menarini, MSD, Mutuam, Novo Nordisk, Pronokal, RedGDPS, Rovi, Sanofi Aventis.</p><p id="par0205" class="elsevierStylePara elsevierViewall">Fernando Gallardo has received fees as presenter, consultant, and support for attendance of course and congresses and/or investigation projects in the following companies: Janssen, Abbvie, UCB, Amgen, Bristol, Lilly, Novartis, Almirall, Leo Pharma.</p><p id="par0210" class="elsevierStylePara elsevierViewall">Antonio Martorell has received fees and/or travel grants and/or acted as a member of the steering committees from Novartis, Abbvie, Janssen Cilag, UCB, Lilly, LEO Pharma, L’Oreal, Sanofi, Boehringer Ingelheim, Almirall, Bristol Myers Squibb, and Amgen. He has also worked as the principal investigator in clinical trials sponsored by Abbvie, UCB, Janssen, Bristol Myers Squibb, Lilly, Galderma, Sanofi, and Novartis.</p><p id="par0215" class="elsevierStylePara elsevierViewall">José Manuel Carrascosa has participated as PI/SI and/or guest presenter and/or advisor for Almirall, Janssen, Abbvie, UCB, Boehringer-Ingelheim, Lilly, Novartis, Amgen, BMS, and Sandoz.</p></span></span>" "textoCompletoSecciones" => array:1 [ "secciones" => array:12 [ 0 => array:3 [ "identificador" => "xres2067373" "titulo" => "Graphical abstract" "secciones" => array:1 [ 0 => array:1 [ "identificador" => "abst0005" ] ] ] 1 => array:3 [ "identificador" => "xres2067372" "titulo" => "Abstract" "secciones" => array:1 [ 0 => array:1 [ "identificador" => "abst0010" ] ] ] 2 => array:2 [ "identificador" => "xpalclavsec1764147" "titulo" => "Keywords" ] 3 => array:3 [ "identificador" => "xres2067374" "titulo" => "Resumen" "secciones" => array:1 [ 0 => array:1 [ "identificador" => "abst0015" ] ] ] 4 => array:2 [ "identificador" => "xpalclavsec1764148" "titulo" => "Palabras clave" ] 5 => array:3 [ "identificador" => "sec0005" "titulo" => "Low-grade chronic inflammation and immunological imbalance facilitate a bidirectional association between obesity and immune-mediated dermatoses" "secciones" => array:2 [ 0 => array:2 [ "identificador" => "sec0010" "titulo" => "Psoriasis and obesity" ] 1 => array:2 [ "identificador" => "sec0015" "titulo" => "Hidradenitis suppurativa and obesity" ] ] ] 6 => array:2 [ "identificador" => "sec0020" "titulo" => "Advantages associated with weight loss in patients with obesity and psoriasis or hidradenitis suppurativa" ] 7 => array:3 [ "identificador" => "sec0025" "titulo" => "Specific treatments for weight loss" "secciones" => array:2 [ 0 => array:2 [ "identificador" => "sec0030" "titulo" => "Diet and exercise" ] 1 => array:3 [ "identificador" => "sec0035" "titulo" => "Approved and marketed drugs in Spain" "secciones" => array:14 [ 0 => array:2 [ "identificador" => "sec0040" "titulo" => "Orlistat" ] 1 => array:2 [ "identificador" => "sec0045" "titulo" => "GLP-1 receptor agonists" ] 2 => array:2 [ "identificador" => "sec0050" "titulo" => "Indications, pleiotropic actions" ] 3 => array:2 [ "identificador" => "sec0055" "titulo" => "GLP-1 receptor agonists in the obesity setting" ] 4 => array:2 [ "identificador" => "sec0060" "titulo" => "Dosing, safety profile" ] 5 => array:2 [ "identificador" => "sec0065" "titulo" => "Arguments in favor of GLP-1 receptor agonists for weight control in patients with obesity and inflammatory dermatoses" ] 6 => array:2 [ "identificador" => "sec0070" "titulo" => "GLP-1 receptor agonists with indication for obesity" ] 7 => array:2 [ "identificador" => "sec0075" "titulo" => "Liraglutide 3 mg" ] 8 => array:2 [ "identificador" => "sec0080" "titulo" => "Semaglutide 2.4 mg" ] 9 => array:3 [ "identificador" => "sec0085" "titulo" => "Experience with liraglutide and semaglutide in psoriasis and hidradenitis suppurativa" "secciones" => array:1 [ 0 => array:2 [ "identificador" => "sec0090" "titulo" => "Liraglutide and psoriasis" ] ] ] 10 => array:2 [ "identificador" => "sec0095" "titulo" => "Semaglutide and psoriasis" ] 11 => array:2 [ "identificador" => "sec0100" "titulo" => "Liraglutide and hidradenitis suppurativa" ] 12 => array:2 [ "identificador" => "sec0105" "titulo" => "Possibilities for use of GLP-1 receptor agonists in Spain for treatment of obesity" ] 13 => array:2 [ "identificador" => "sec0110" "titulo" => "Other medium-term therapeutic options" ] ] ] ] ] 8 => array:2 [ "identificador" => "sec0115" "titulo" => "Conclusions" ] 9 => array:2 [ "identificador" => "sec0120" "titulo" => "Funding" ] 10 => array:2 [ "identificador" => "sec0125" "titulo" => "Conflicts of Interest" ] 11 => array:1 [ "titulo" => "References" ] ] ] "pdfFichero" => "main.pdf" "tienePdf" => true "fechaRecibido" => "2023-05-11" "fechaAceptado" => "2023-06-28" "PalabrasClave" => array:2 [ "en" => array:1 [ 0 => array:4 [ "clase" => "keyword" "titulo" => "Keywords" "identificador" => "xpalclavsec1764147" "palabras" => array:6 [ 0 => "Psoriasis" 1 => "Hidradenitis suppurativa" 2 => "Obesity" 3 => "Glucagon-like peptide-1 (GLP-1) agonists" 4 => "Liraglutide" 5 => "Semaglutide" ] ] ] "es" => array:1 [ 0 => array:4 [ "clase" => "keyword" "titulo" => "Palabras clave" "identificador" => "xpalclavsec1764148" "palabras" => array:6 [ 0 => "Psoriasis" 1 => "Hidradenitis supurativa" 2 => "Obesidad" 3 => "Agonistas del receptor de GLP-1" 4 => "Liraglutida" 5 => "Semaglutida" ] ] ] ] "tieneResumen" => true "resumen" => array:2 [ "en" => array:2 [ "titulo" => "Abstract" "resumen" => "<span id="abst0010" class="elsevierStyleSection elsevierViewall"><p id="spar0010" class="elsevierStyleSimplePara elsevierViewall">Psoriasis and hidradenitis suppurativa are often associated with obesity. Because chronic low-grade inflammation underlies these 2 diseases, they can progress to more severe forms in patients with obesity if weight-reduction measures are not taken. This review covers pharmacologic alternatives for treating obesity, with emphasis on the benefits associated with the novel use of glucagon-like peptide-1 (GLP-1) agonists that act on satiety receptors. These drugs have led to greater weight loss in clinical trials and real-world settings than orlistat, which until recently was the only drug approved for treating obesity in the European Union. Although experience with GLP-1 agonists in patients with obesity and inflammatory skin diseases is currently scarce, the promising results reported suggest they may offer a useful tool for managing obesity.</p></span>" ] "es" => array:2 [ "titulo" => "Resumen" "resumen" => "<span id="abst0015" class="elsevierStyleSection elsevierViewall"><p id="spar0015" class="elsevierStyleSimplePara elsevierViewall">La psoriasis (PsO) y la hidradenitis supurativa (HS) se asocian frecuentemente con la obesidad. La inflamación crónica de bajo grado subyace a estas condiciones, por lo que si no se adoptan medidas para reducir el peso del paciente con obesidad y PsO o HS, estas podrían evolucionar hacia formas más graves. Este trabajo revisa las opciones farmacológicas para tratar la obesidad, profundizando en los beneficios asociados al uso novedoso de agonistas del receptor de GLP-1 (arGLP-1), que actúan sobre los centros de la saciedad. Los resultados de ensayos y vida real demuestran que esta medicación consigue mayores pérdidas de peso que orlistat, hasta recientemente el único fármaco específico para la obesidad comercializado en la Unión Europea. Aunque la experiencia con arGLP-1 en pacientes con obesidad y dermatosis inflamatorias es escasa, los resultados son alentadores, por lo que podrían constituir una herramienta útil para el manejo de su obesidad.</p></span>" ] ] "apendice" => array:1 [ 0 => array:1 [ "seccion" => array:1 [ 0 => array:4 [ "apendice" => "<p id="par0225" class="elsevierStylePara elsevierViewall"><elsevierMultimedia ident="upi0005"></elsevierMultimedia></p>" "etiqueta" => "Appendix B" "titulo" => "Additional material" "identificador" => "sec0135" ] ] ] ] "multimedia" => array:5 [ 0 => array:7 [ "identificador" => "fig0005" "etiqueta" => "Figure 1" "tipo" => "MULTIMEDIAFIGURA" "mostrarFloat" => true "mostrarDisplay" => false "figura" => array:1 [ 0 => array:4 [ "imagen" => "gr1.jpeg" "Alto" => 2428 "Ancho" => 2508 "Tamanyo" => 427081 ] ] "descripcion" => array:1 [ "en" => "<p id="spar0020" class="elsevierStyleSimplePara elsevierViewall">Pleiotropic effect of GLP-1 receptor agonists. The effects of GLP-1 receptor agonists on different organs and, in red, their consequences.</p> <p id="spar0025" class="elsevierStyleSimplePara elsevierViewall">*Glucose-dependent biosynthesis and secretion. †Glucose-dependent secretion.</p> <p id="spar0030" class="elsevierStyleSimplePara elsevierViewall">Abbreviations: AMI: acute myocardial infarction; BP: blood pressure; CVA: cerebrovascular accident; FA fatty acids; GLP-1 ra glucagon-like protein-1 receptor agonist; IR: insulin resistance.</p>" ] ] 1 => array:7 [ "identificador" => "fig0010" "etiqueta" => "Figure 2" "tipo" => "MULTIMEDIAFIGURA" "mostrarFloat" => true "mostrarDisplay" => false "figura" => array:1 [ 0 => array:4 [ "imagen" => "gr2.jpeg" "Alto" => 1980 "Ancho" => 1672 "Tamanyo" => 139451 ] ] "descripcion" => array:1 [ "en" => "<p id="spar0035" class="elsevierStyleSimplePara elsevierViewall">Decision tree for use of GLP-1 receptor agonists indicated for weight control in patients with obesity or excess weight with comorbidities. Different possibilities are considered depending on whether the patient is obese (BMI≥ 30<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>) or overweight (BMI≥ 27- <<span class="elsevierStyleHsp" style=""></span>30<span class="elsevierStyleHsp" style=""></span>kg/m<span class="elsevierStyleSup">2</span>) with ≥ 1 weight-related comorbidity. These therapeutic options can be used for weight control in patients with immune-mediated dermatosis who meet the above criteria. Semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg, although approved by the EMA and AEMPS, has still not been marketed in Spain.</p> <p id="spar0040" class="elsevierStyleSimplePara elsevierViewall">* At least 1 weight-related comorbidity: in the case of liraglutide 3<span class="elsevierStyleHsp" style=""></span>mg, poor glycemic control (prediabetes or DT2), hypertension, dyslipidemia or sleep obstructive apnea; in the case of semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg, glucose disorder (prediabetes or DT2), hypertension, dyslipidemia, sleep obstructive apnea, or cardiovascular disease.</p> <p id="spar0045" class="elsevierStyleSimplePara elsevierViewall">† 3<span class="elsevierStyleHsp" style=""></span>mg, daily, subcutaneous administration, in monotherapy or in combination with other medications.</p> <p id="spar0050" class="elsevierStyleSimplePara elsevierViewall">‡ 1.8<span class="elsevierStyleHsp" style=""></span>mg, daily, subcutaneous administration, in monotherapy or in combination with other medications.</p> <p id="spar0055" class="elsevierStyleSimplePara elsevierViewall">Abbreviations: AEMPS: Spanish Agency for Drugs and Medicinal Products; BMI: body mass index; DT2: type 2 diabetes; EMA: European Medicines Agency; GLP-1: glucagon-like peptide 1 receptor; HS: hidradenitis suppurativa; MET: metformin; PsO: psoriasis.</p>" ] ] 2 => array:8 [ "identificador" => "tbl0005" "etiqueta" => "Table 1" "tipo" => "MULTIMEDIATABLA" "mostrarFloat" => true "mostrarDisplay" => false "detalles" => array:1 [ 0 => array:3 [ "identificador" => "at1" "detalle" => "Table " "rol" => "short" ] ] "tabla" => array:3 [ "leyenda" => "<p id="spar0065" class="elsevierStyleSimplePara elsevierViewall">Abbreviations: AEs, adverse events; BMI, body mass index at baseline; Pl: placebo; SID, once daily.</p>" "tablatextoimagen" => array:1 [ 0 => array:2 [ "tabla" => array:1 [ 0 => """ <table border="0" frame="\n \t\t\t\t\tvoid\n \t\t\t\t" class=""><thead title="thead"><tr title="table-row"><th class="td" title="\n \t\t\t\t\ttable-head\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t" scope="col" style="border-bottom: 2px solid black">Trial \t\t\t\t\t\t\n \t\t\t\t\t\t</th><th class="td" title="\n \t\t\t\t\ttable-head\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t" scope="col" style="border-bottom: 2px solid black">SCALE Obesity<a class="elsevierStyleCrossRef" href="#bib0780"><span class="elsevierStyleSup">69</span></a> \t\t\t\t\t\t\n \t\t\t\t\t\t</th><th class="td" title="\n \t\t\t\t\ttable-head\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t" scope="col" style="border-bottom: 2px solid black">SCALE Maintenance<a class="elsevierStyleCrossRef" href="#bib0785"><span class="elsevierStyleSup">70</span></a> \t\t\t\t\t\t\n \t\t\t\t\t\t</th><th class="td" title="\n \t\t\t\t\ttable-head\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t" scope="col" style="border-bottom: 2px solid black">STEP 1<a class="elsevierStyleCrossRef" href="#bib0820"><span class="elsevierStyleSup">77</span></a> \t\t\t\t\t\t\n \t\t\t\t\t\t</th><th class="td" title="\n \t\t\t\t\ttable-head\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t" scope="col" style="border-bottom: 2px solid black">STEP 3<a class="elsevierStyleCrossRef" href="#bib0825"><span class="elsevierStyleSup">78</span></a> \t\t\t\t\t\t\n \t\t\t\t\t\t</th><th class="td" title="\n \t\t\t\t\ttable-head\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t" scope="col" style="border-bottom: 2px solid black">STEP 4<a class="elsevierStyleCrossRef" href="#bib0815"><span class="elsevierStyleSup">76</span></a> \t\t\t\t\t\t\n \t\t\t\t\t\t</th></tr></thead><tbody title="tbody"><tr title="table-row"><td class="td-with-role" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t ; entry_with_role_rowhead " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Duration, weeks \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">56 \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Preinclusion<a class="elsevierStyleCrossRef" href="#tblfn0005">*</a> +<span class="elsevierStyleHsp" style=""></span>56 \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">68 \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">68 \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">68 \t\t\t\t\t\t\n \t\t\t\t</td></tr><tr title="table-row"><td class="td-with-role" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t ; entry_with_role_rowhead " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Group<span class="elsevierStyleSup">a</span> \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Liraglutide 3 mg vs. Pl (2:1) \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Liraglutide 3 mg vs. Pl (1:1) \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg vs. Pl (2:1) \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg vs. Pl (2:1) \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg vs. Pl (2:1)<a class="elsevierStyleCrossRef" href="#tblfn0010"><span class="elsevierStyleSup">†</span></a> \t\t\t\t\t\t\n \t\t\t\t</td></tr><tr title="table-row"><td class="td-with-role" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t ; entry_with_role_rowhead " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Design \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Randomized/double blind \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">• <span class="elsevierStyleItalic">Run-in: diet +</span><span class="elsevierStyleHsp" style=""></span><span class="elsevierStyleItalic">exercise</span>• <span class="elsevierStyleItalic">Week 0-56:</span> randomized/double blind, liraglutide 3 mg or Pl \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Randomized/double blind \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Randomized/double blind \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">• <span class="elsevierStyleItalic">Week 0-20 (run-in)</span>:semaglutide• <span class="elsevierStyleItalic">Week 20-68¡</span>: randomized/doubleblind, semaglutide or Pl \t\t\t\t\t\t\n \t\t\t\t</td></tr><tr title="table-row"><td class="td-with-role" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t ; entry_with_role_rowhead " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Patients (n; BMI<span class="elsevierStyleSup">b</span>) \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">3731; 38.3 kg/m<span class="elsevierStyleSup">2</span> \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">422; 37.8 kg/m<span class="elsevierStyleSup">2</span> \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">1961; 37.9 kg/m<span class="elsevierStyleSup">2</span> \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">611; 38.0 kg/m<span class="elsevierStyleSup">2</span> \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">803; 38.4 kg/m<span class="elsevierStyleSup">2</span> \t\t\t\t\t\t\n \t\t\t\t</td></tr><tr title="table-row"><td class="td-with-role" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t ; entry_with_role_rowhead " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Therapeutic regimen \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Liraglutide 3 mg SID vs. Pl (plus lifestyle intervention) \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">• <span class="elsevierStyleItalic">Run-in:</span> low calory diet +<span class="elsevierStyleHsp" style=""></span>exercise• <span class="elsevierStyleItalic">Week 0-56:</span> liraglutide 3 mg SID vs. Pl \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg/week vs. Pl (plus lifestyle intervention) \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg/week vs. Pl (+ lifestyle intervention +<span class="elsevierStyleHsp" style=""></span>low-calory diet in weeks 1-8) \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">• <span class="elsevierStyleItalic">Week 0-20:</span> semaglutide 2.4 mg/week• <span class="elsevierStyleItalic">Week 21-68:</span> semaglutide 2.4 mg/week vs. Pl \t\t\t\t\t\t\n \t\t\t\t</td></tr><tr title="table-row"><td class="td-with-role" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t ; entry_with_role_rowhead " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Weight loss, % \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Liraglutide 3 mg: -8.0%, Pl: 2.6% \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">• <span class="elsevierStyleItalic">Run-in:</span>Liraglutide 3 mg: -5.9%,Pl -6%• <span class="elsevierStyleItalic">From randomization until 56 weeks later:</span>Liraglutide 3 mg: -6.2%,Pl -0.2% \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg: -14.9%, Pl: -2.4% \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg: -16.0%,Pl: -5.7% \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">• <span class="elsevierStyleItalic">Week 0-68:</span> semaglutide 2.4 mg:-17.4%, Pl: -5.0%• <span class="elsevierStyleItalic">Week 20-68:</span> semaglutide 2.4 mg:-7.9%, Pl: +<span class="elsevierStyleHsp" style=""></span>6.2% \t\t\t\t\t\t\n \t\t\t\t</td></tr><tr title="table-row"><td class="td-with-role" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t ; entry_with_role_rowhead " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Discontinuation due to AEs<a class="elsevierStyleCrossRef" href="#tblfn0015"><span class="elsevierStyleSup">‡</span></a> \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Liraglutide 3 mg: 9.9%,Pl: 3.8% \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Liraglutide 3 mg: 8.5%, Pl: 8.6% \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg: 7.0%, Pl: 3.1% \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">Semaglutide 2.4 mg: 5.9%, Pl: 2.9% \t\t\t\t\t\t\n \t\t\t\t</td><td class="td" title="\n \t\t\t\t\ttable-entry\n \t\t\t\t " align="left" valign="\n \t\t\t\t\ttop\n \t\t\t\t">• <span class="elsevierStyleItalic">Week 0-20:</span> semaglutide 2.4 mg: 5.3%• <span class="elsevierStyleItalic">Week 20-68:</span> semaglutide 2.4 mg: 2.4%, Pl: 2.2% \t\t\t\t\t\t\n \t\t\t\t</td></tr></tbody></table> """ ] "imagenFichero" => array:1 [ 0 => "xTab3424689.png" ] ] ] "notaPie" => array:3 [ 0 => array:3 [ "identificador" => "tblfn0005" "etiqueta" => "*" "nota" => "<p class="elsevierStyleNotepara" id="npar0005">In the run-in period, all patients, regardless of whether we are randomized to receive lira or placebo later, were subject to a hypocaloric diet and exercise regime, without GLP-1 receptor agonist, with the duration of the period for each patient being the time required to lose ≥<span class="elsevierStyleHsp" style=""></span>5% of their baseline body weight</p>" ] 1 => array:3 [ "identificador" => "tblfn0010" "etiqueta" => "†" "nota" => "<p class="elsevierStyleNotepara" id="npar0010">In the run-in period, all patients received semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg, and from week 20 they were randomized in a 2:1 ratio to continue with semaglutide 2.4<span class="elsevierStyleHsp" style=""></span>mg or receive placebo.</p>" ] 2 => array:3 [ "identificador" => "tblfn0015" "etiqueta" => "‡" "nota" => "<p class="elsevierStyleNotepara" id="npar0015">The AEs reported were mainly gastrointestinal in nature, in particular nausea, although diarrhea, vomiting, and occasionally constipation, were also reported.</p>" ] ] ] "descripcion" => array:1 [ "en" => "<p id="spar0060" class="elsevierStyleSimplePara elsevierViewall">Phase 3 trials with GLP-1 receptor agonists indicated specifically for obesity and overweight.</p>" ] ] 3 => array:5 [ "identificador" => "upi0005" "tipo" => "MULTIMEDIAECOMPONENTE" "mostrarFloat" => false "mostrarDisplay" => true "Ecomponente" => array:2 [ "fichero" => "mmc1.pdf" "ficheroTamanyo" => 322088 ] ] 4 => array:5 [ "identificador" => "fig0015" "tipo" => "MULTIMEDIAFIGURA" "mostrarFloat" => false "mostrarDisplay" => true "figura" => array:1 [ 0 => array:4 [ "imagen" => "fx1.jpeg" "Alto" => 1085 "Ancho" => 753 "Tamanyo" => 71948 ] ] ] ] "bibliografia" => array:2 [ "titulo" => "References" "seccion" => array:1 [ 0 => array:2 [ "identificador" => "bibs0015" "bibliografiaReferencia" => array:87 [ 0 => array:3 [ "identificador" => "bib0440" "etiqueta" => "1" "referencia" => array:1 [ 0 => array:2 [ "contribucion" => array:1 [ 0 => array:2 [ "titulo" => "Revisiting the adipocyte: a model for integration of cytokine signaling in the regulation of energy metabolism" "autores" => array:1 [ 0 => array:2 [ "etal" => false "autores" => array:5 [ …5] ] ] ] ] "host" => array:1 [ 0 => array:2 [ "doi" => "10.1152/ajpendo.00297.2015" "Revista" => array:6 [ "tituloSerie" => "Am J Physiol Endocrinol Metab." 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año/Mes | Html | Total | |
---|---|---|---|
2024 Noviembre | 11 | 1 | 12 |
2024 Octubre | 183 | 119 | 302 |
2024 Septiembre | 177 | 119 | 296 |
2024 Agosto | 212 | 137 | 349 |
2024 Julio | 200 | 129 | 329 |
2024 Junio | 158 | 129 | 287 |
2024 Mayo | 139 | 93 | 232 |
2024 Abril | 155 | 89 | 244 |
2024 Marzo | 164 | 97 | 261 |
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2024 Enero | 399 | 121 | 520 |
2023 Diciembre | 138 | 78 | 216 |
2023 Noviembre | 170 | 104 | 274 |