ライフサイエンスコーパス: immunosuppression

1 a treatment option in sepsis associated with immunosuppression.

2 ncreas tissue and (b) the need for life-long immunosuppression.

3 acept-based, compared with tacrolimus-based, immunosuppression.

4 ge and limits extrinsic myeloid and lymphoid immunosuppression.

5 orted by RANK-expressing tumor cells, induce immunosuppression.

6 omplicated infection (eg, abscess) or severe immunosuppression.

7 buting to both immune homeostasis and cancer immunosuppression.

8 nomodulator were frail in the 2 years before immunosuppression.

9 , on tumor-infiltrating leukocytes eliciting immunosuppression.

10 umorigenicity and lung metastasis is through immunosuppression.

11 tumor effects and to inhibit surgery-induced immunosuppression.

12 higher risk for long-term complications from immunosuppression.

13 ted in cancers to inhibit T cells and elicit immunosuppression.

14 medical advice, the patient discontinued all immunosuppression.

15 not receive a transplant (11.6%) are without immunosuppression.

16 immunosuppression.

17 ical technique, type of donor, and induction immunosuppression.

18 in 28.5% of the cases after minimization of immunosuppression.

19 cancer, independently from age, gender, and immunosuppression.

20 antation in addition to post-transplantation immunosuppression.

21 d tacrolimus for partial lymphocyte-directed immunosuppression.

22 prolong graft function and elicit localized immunosuppression.

23 B1 and is important for T(reg) cell-mediated immunosuppression.

24 ystem, early surgery, indwelling devices, or immunosuppression.

25 rrhosis had excessive alcohol consumption or immunosuppression.

26 900 days, with rejection only after reducing immunosuppression.

27 into consideration the potential effects of immunosuppression.

28 transplant to minimise the burden of general immunosuppression.

29 acellular matrix remodelling, metastasis and immunosuppression.

30 rejection and the requirement for long-term immunosuppression.

31 They are linked by the net state of immunosuppression.

32 impair nanomedicine delivery can also cause immunosuppression.

33 ature with upregulation of genes involved in immunosuppression.

34 hesized that IL17 triggers and sustains PDAC immunosuppression.

35 ic infections attributable to induced global immunosuppression.

36 0 copies/ml that resolved after reduction of immunosuppression.

37 transplant model in the absence of exogenous immunosuppression.

38 demonstrated a dramatic clinical response to immunosuppression.

39 from latency beyond their general effects on immunosuppression.

40 epatocytes were rejected but engrafted after immunosuppression.

41 odies, but they are unresponsive to standard immunosuppression.

42 mal tumor microenvironment (TME)-that causes immunosuppression.

43 monitored closely in the setting of lowered immunosuppression.

44 key diabetes-related genes in the context of immunosuppression.

45 imilar risks across strata of viral load and immunosuppression.

46 T (iNKT) cells with glycolipid antigen drove immunosuppression.

47 -host disease (GVHD) results from inadequate immunosuppression.

48 e used to guide personalized post-transplant immunosuppression.

49 thus, contribute to tumor proliferation and immunosuppression.

50 ft thickness in a murine model of transplant immunosuppression.

51 tation of engineered cells in the absence of immunosuppression.

52 robial constituents promote inflammation and immunosuppression.

53 ontrols islet autoimmunity without long-term immunosuppression.

54 male Mecp2 mutant mice that was overcome by immunosuppression.

55 for treatment thereby removing the need for immunosuppression.

56 nfection, cancer, and other complications of immunosuppression.

57 ons in markers and cytokines associated with immunosuppression.

58 he Cxcl8 pathway exhibited dominance despite immunosuppression.

59 life-threatening infections due to lifelong immunosuppression.

60 ent-dependent cytotoxicity through relief of immunosuppression.

61 he potential to obviate the need for chronic immunosuppression.

62 ed therapeutic interventions such as reduced immunosuppression.

63 nucleosis that showed a dramatic response to immunosuppression.

64 months following a standardized reduction in immunosuppression.

65 ion corresponded with indicators of systemic immunosuppression.

66 compare outcomes of SLKT, based on induction immunosuppression.

67 by activating cellular pathways that lead to immunosuppression.

68 sistant bacteria-induced sepsis in mice with immunosuppression.

69 tional tolerance after complete cessation of immunosuppression.

70 togenic genes dysregulated in the context of immunosuppression.

71 ted with increased mortality and features of immunosuppression.

72 r promotion by severe, prolonged HIV-induced immunosuppression.

73 on of Treg in AA, which predicts response to immunosuppression.

74 tore self-tolerance without inducing chronic immunosuppression.

75 rvival depends on reversal of the underlying immunosuppression.

76 ieving transplantation without the requisite immunosuppression.

77 Most were male (95; 65.5%) and had immunosuppression (120; 82.8%), including solid organ tr

78 Reduction in immunosuppression (49.4%) was not associated with liver

79 ptophan 2,3-dioxygenase 2 (IDO/TDO) promotes immunosuppression across different cancer types.

80 ologic response rates even in the setting of immunosuppression after transplantation, these HCV-virem

81 is insufficient to estimate the intensity of immunosuppression after transplantation.

82 ne cells [MICs]), induced long-term specific immunosuppression against the allogeneic donor.METHODSIn

83 steroidogenesis as a mechanism of anti-tumor immunosuppression and a potential druggable target.

84 9 due the high prevalence of co-morbidities, immunosuppression and ageing, a detailed analysis of the

85 es are being studied(7), which often involve immunosuppression and are not efficient in removing pre-

86 sease 2019 (COVID-19) illness due to chronic immunosuppression and comorbidities.

87 ompared to nontransplant patients because of immunosuppression and comorbidities.

88 most significantly upregulated genes in both immunosuppression and diabetes subsets and were appropri

89 transplantation (HT), where the advances in immunosuppression and donor selection strategies have le

90 d STING agonists could help to reduce tumour immunosuppression and enhance the efficacy of a wide ran

91 TANCE Chronic viral infections may result in immunosuppression and enhanced susceptibility to infecti

92 CDH11 promotes immunosuppression and extracellular matrix deposition, a

93 The relative immunosuppression and high prevalence of comorbidities i

94 in vivo mechanisms underlying sepsis-induced immunosuppression and identify TNFR2pos Treg as targets

95 In addition to established risk factors (immunosuppression and infectious mononucleosis), allergi

96 Kgamma constitutes an opportunity to mediate immunosuppression and inflammation within the tumor micr

97 Rubcn(-/-) mice are resistant to UV-induced immunosuppression and instead display exaggerated inflam

98 However, the requirement for life-long immunosuppression and its associated side effects preclu

99 had a favorable disease course, but some had immunosuppression and liver cirrhosis.

100 Thus, PTGES/PGE(2) signaling links immunosuppression and metastasis in an inflammatory lung

101 strate that brain cancers cause multifaceted immunosuppression and pinpoint circulating factors as a

102 /TA-encapsulated islets can elicit localized immunosuppression and potentially delay graft destructio

103 is the most important agent for maintenance immunosuppression and prevention of immunologic injury t

104 lant and patient outcomes due to advances in immunosuppression and prevention of posttransplantation

105 observed, most likely due to advancements in immunosuppression and preventive strategies, including p

106 In the current era of immunosuppression and prophylaxis, SOT recipients experi

107 rehensively documented in the current era of immunosuppression and prophylaxis.

108 -cleaving Cas nucleases, which cause limited immunosuppression and require multiple infections to byp

109 felong disease activity, implying a need for immunosuppression and risk of malignancy, must be weighe

110 matory phase of sepsis improves, post-sepsis immunosuppression and secondary infection have increased

111 d acute rejection correlates with troughs in immunosuppression and subsides when immunosuppressive ta

112 e or inhibition of mTOR by rapamycin reduced immunosuppression and susceptibility to secondary Candid

113 onstrate that LAP is required for UV-induced immunosuppression and that UV exposure induces a broadly

114 Despite reduction in immunosuppression and treatment with tocilizumab, intrav

115 In the era of contemporary immunosuppression and valganciclovir prophylaxis, a sign

116 t can lead to minimization or elimination of immunosuppression and, it is hoped, help revitalize the

117 of tacrolimus/mammalian target of rapamycin immunosuppression, and an acute rejection event were ind

118 regulatory T (Treg)-cells, where it mediates immunosuppression, and by a subset of T-helper (Th) 17-c

119 y recapitulates the persistent inflammation, immunosuppression, and catabolism syndrome observed in a

120 CTLA-4 is a key molecule in immunosuppression, and CD80 is a costimulatory receptor

121 ion, but the procedure is invasive, requires immunosuppression, and could cause other complications s

122 ase, lung disease, kidney disease, diabetes, immunosuppression, and liver disease were associated wit

123 transplantation, affecting donor selection, immunosuppression, and posttransplant management.

124 lection, donor and HTx recipient management, immunosuppression, and pretransplant mechanical circulat

125 stic response that promotes hypovascularity, immunosuppression, and resistance to chemo- and immunoth

126 er the expansion of those cells that survive immunosuppression, and this expansion could be associate

127 Clinical presentation, laboratory values, immunosuppression, and treatment strategies were reviewe

128 nse, tests for quantifying the "net state of immunosuppression," and genetic polymorphisms associated

129 Diagnostic workup, clinical course, immunosuppression/antiviral management, and immediate ou

130 icantly dysregulated genes in the context of immunosuppression are implicated in insulin signaling an

131 rent paramyxoviruses, like neurotoxicity and immunosuppression, are now understood in the light of re

132 transformed cells, resulting in significant immunosuppression-associated comorbidities.

133 ge was 6.4 years and 68% had advanced/severe immunosuppression at ART initiation.

134 lects meticulous attention to the details of immunosuppression, balancing risks for graft rejection a

135 to Tac withdrawal or maintenance of standard immunosuppression beginning 6 months after transplant.

136 Ms promote tumor-associated angiogenesis and immunosuppression by altering metabolism in breast cance

137 ese findings characterize a new mechanism of immunosuppression by hypoxia via downregulation of the t

138 reduced due to immunological immaturity and immunosuppression by RSV-specific maternal antibodies.

139 Immunosuppression by systemic CsA, but not UV-B irradiat

140 ts have been made to circumvent the need for immunosuppression by using various techniques to achieve

141 ting the expression of genes associated with immunosuppression, chemotaxis, and tumor matrix remodeli

142 ults provide a possible mechanism behind the immunosuppression commonly seen in breast cancer patient

143 Immunosuppression consisted of basiliximab, tacrolimus,

144 Immunosuppression continues to be a necessary component

145 such as bacterial or viral coinfections and immunosuppression (corticosteroids).

146 We hypothesized that patients with advanced immunosuppression could be stratified into inflammatory

147 In a threshold analysis, the extension of immunosuppression coverage was cost-effective at a willi

148 graft survival in the absence of continuing immunosuppression, defined as operational tolerance, has

149 We demonstrate that IDO-Kyn-AHR-mediated immunosuppression depends on an interplay between Tregs

150 Immunosuppression devoid of corticosteroids has been inv

151 In the absence of systemic immunosuppression, diabetic recipients containing PVPON/

152 Metastasis is a molecularly late event, and immunosuppression driven by different molecular events,

153 tment with corticosteroids and a second-line immunosuppression drug and treated with biologic agents

154 tment with corticosteroids and a second-line immunosuppression drug experienced satisfactory disease

155 Few studies address adjustment of immunosuppression during active infections.

156 the oncolytic virus overcomes PD-L1-mediated immunosuppression during both the priming and effector p

157 Reduction of immunosuppression during COVID-19 did not increase risk

158 Group C patients with low immunosuppression during follow-up showed no in vitro re

159 a conceptual framework for the management of immunosuppression during infection in organ recipients.

160 warranted to assess the optimal maintenance immunosuppression during the use of checkpoint inhibitor

161 mplicated an NKT cell/mTOR/IFN-gamma axis in immunosuppression following endotoxemia or sepsis.

162 cribed the use of sirolimus (SRL) as primary immunosuppression following heart transplantation (HT).

163 the reduction or complete discontinuation of immunosuppression following liver transplantation.

164 mi-allogeneic graft that can survive without immunosuppression for 9 months.

165 as World Health Organization advanced/severe immunosuppression for age) at 1 year of VS was described

166 P prophylaxis in those receiving intensified immunosuppression for graft rejection, CMV infection, hi

167 engraftment, and to those receiving systemic immunosuppression for graft-versus-host disease treatmen

168 between frailty and risk of infections after immunosuppression for IBD.

169 There is scant data on the use of induction immunosuppression for simultaneous liver/kidney transpla

170 ft, despite the avoidance of antibiotics and immunosuppression for the latter.

171 Here, we discuss the management of immunosuppression for these patients during the pandemic

172 nfections are an important adverse effect of immunosuppression for treatment of inflammatory bowel di

173 on to test strategies that promote long-term immunosuppression-free allograft survival.

174 CNI-based mammalian target of rapamycin-free immunosuppression (group A, n = 264) was compared with a

175 ith the following criteria: tacrolimus-based immunosuppression, >1-year graft survival, no initial us

176 1.08, 1.7]; P < 0.05) CONCLUSION.: Induction immunosuppression had no impact on patient and allograft

177 New surgical techniques and conventional immunosuppression have enabled some success, but outcome

178 splantation (1.7-4.6-fold) in the absence of immunosuppression, homed to allografts, and suppressed p

179 The mechanisms that underlie immunosuppression, however, remain largely unknown.

180 Immunosuppression improved the HRCT scan scores in patie

181 ant or systemic therapy (corticosteroid plus immunosuppression in >90%) were followed prospectively f

182 dom from rejection following withdrawal from immunosuppression in a clinical trial of kidney transpla

183 ejection because of unnecessary reduction of immunosuppression in case of self-limiting BKPyV-DNAemia

184 ndependent manner, which could contribute to immunosuppression in hypoxic tumors.

185 ogenous virus and is linked to neoplasia and immunosuppression in koalas.

186 We observed no immunosuppression in mice pretreated with natural EVs, w

187 ratio of ADO/AMP significantly and reversed immunosuppression in mouse models, indicating its potent

188 made in understanding immune dysfunction and immunosuppression in multiple myeloma (MM), and various

189 sor cells (G-MDSCs) promote tumor growth and immunosuppression in multiple myeloma (MM).

190 ate-of-the-art approach for reducing general immunosuppression in organ transplantation.

191 ne response: nanodendritic cell vaccines and immunosuppression in ovarian cancer.

192 Frailty was associated with infections after immunosuppression in patients with IBD after we adjust f

193 (MLVI), a surrogate measure of adherence to immunosuppression in pediatric liver transplant recipien

194 Interestingly, the factor responsible for immunosuppression in serum is non-steroidal and of high

195 ate for the first time that CDDO-Me relieves immunosuppression in the breast TME and unleashes host a

196 ove to have unique clinical consequences for immunosuppression in the growing population of elderly t

197 Standard-of-care immunosuppression in the recipients in the RGT resulted

198 crophages and Tregs contributes to potential immunosuppression in the TME.

199 ote the delivery of nanomedicines and reduce immunosuppression in the TME.

200 Thus, a common mechanism underlies immunosuppression in the tumor microenvironment irrespec

201 thymic involution was a hallmark feature of immunosuppression in three distinct models of brain canc

202 d effect of repeated GEM treatment promoting immunosuppression in TME via upregulation of GM-CSF and

203 ntrolled a molecular program responsible for immunosuppression in tumors.

204 ), for macrophage modulation and reversal of immunosuppression in tumors.

205 ponses, balancing inflammatory processes and immunosuppression; indeed, alterations in extracellular

206 For PLWH with severe immunosuppression initiating ART, baseline low BMI and h

207 Multiple measures of immunosuppression intensity were not associated with mor

208 Age and underlying comorbidities rather than immunosuppression intensity-related measures were major

209 This immunosuppression is a critical barrier to the successfu

210 utopsy cases and animal models confirms that immunosuppression is also present in extracranial metast

211 Belatacept-based maintenance immunosuppression is associated with an increased risk o

212 in solid organ recipients, the management of immunosuppression is based largely on clinical experienc

213 system malfunction after allergic disease or immunosuppression is central to HL development.

214 While effective, current immunosuppression is imperfect as it lacks specificity a

215 A consequence of the need for this permanent immunosuppression is the high risk of opportunistic, com

216 -2) adaptive immune response despite chronic immunosuppression is unknown and has important implicati

217 cells (Treg) are involved in this postseptic immunosuppression is unknown.

218 donor, biochemical and clinical data at LT, immunosuppression (IS) and outcome.

219 Maintenance immunosuppression (IS) consisted of sirolimus and mycoph

220 therapy might allow for increased success of immunosuppression (IS) withdrawal.

221 ents, the primary treatment was reduction in immunosuppression (IS).

222 Immunosuppression lasted only for the duration of the ut

223 Refractory cellular immune responses, immunosuppression-linked infections, and posttransplant

224 een mostly focused in countering MDSC-driven immunosuppression, little is known about the mechanisms

225 e risk of alloimmune injury that would guide immunosuppression management in renal transplant patient

226 about the presentation, clinical course, and immunosuppression management of this novel infection amo

227 oimmune risk and may help guide personalized immunosuppression management.

228 transplant recipients treated by belatacept immunosuppression may be at increased risk for Cytomegal

229 Extension of immunosuppression Medicare coverage for kidney transplan

230 s, infliximab dosage information, additional immunosuppression medications, and numbers of and times

231 o cancer therapy, tumor relapse, malignancy, immunosuppression, metastasis, cancer stem cell producti

232 vide an update on the progress of studies of immunosuppression minimization or withdrawal in solid or

233 cells, or macrophages; patient selection and immunosuppression mirrored the RGT, except basiliximab i

234 We recapitulated the immunosuppression observed in glioblastoma patients in t

235 rofile at the DTH biopsy site corresponds to immunosuppression of an Ag-induced T cell response.

236 hy seen at our center in three patients with immunosuppression of different origins: one with stage I

237 or knockdown of GM-CSF can partially reduce immunosuppression of Ly6C(high) cells induced by GEM-con

238 Immunosuppression of unknown aetiology is a hallmark fea

239 s high sensitivity for the detection of over-immunosuppression (OIS) events.

240 s well as the limited data on the effects of immunosuppression on cancer-specific outcomes.

241 the cases arise in the background of chronic immunosuppression or immune dysregulation.

242 [1.04-1.46]; P = 0.01), and minimization of immunosuppression (OR, 26.2 [5.48-166.6]; P < 0.001).

243 hibitor therapy is effective for maintenance immunosuppression, our preliminary data suggest that eve

244 correlated these data points to clinical and immunosuppression parameters.

245 t clinical consequences, including prolonged immunosuppression, poor vaccine responses and increased

246 mplex patients given their high net state of immunosuppression prior to CAR-T-cell infusion coupled w

247 lar adenosine/A2 adenosine receptor-mediated immunosuppression protects tissues from collateral damag

248 A 10 day steroid-based immunosuppression protocol and a splenectomy at the time

249 Current immunosuppression protocols are not designed to target a

250 Despite recent advances in immunosuppression protocols, allograft damage inflicted

251 Patients were managed with immunosuppression reduction and the addition of hydroxyc

252 mbining low-dose EVL and CNIs in maintenance immunosuppression regimen (quadritherapy) and compare it

253 er a delayed (ie, 28 +/- 4 d posttransplant) immunosuppression regimen based on everolimus (EVR) redu

254 s regarding recurrence prevention, including immunosuppression regimen or secondary prevention with a

255 ng-term deleterious effects of combinatorial immunosuppression regimens and allograft failure cause s

256 types, donor creatinine, ischemic time, and immunosuppression regimens.

257 How early inflammation drives immunosuppression remains unclear.

258 ave a high percentage of failure and lead to immunosuppression, repair GPCRs have promising therapeut

259 me to relieve early immunopathology and late immunosuppression, respectively.

260 Treatment protocol consisted of reduction of immunosuppression (RIS), rituximab (from 2000), cytotoxi

261 However, the mechanisms of immunosuppression selective to Treg cells in patients wi

262 Minimization of immunosuppression should be done with caution in LR HLAi

263 ukoencephalopathy, regardless of the type of immunosuppression, so this finding should routinely asse

264 ase control (87.2%), reduced use of systemic immunosuppression, stable visual acuity, and a 23.7% ris

265 observed in those patients having underlying immunosuppression such as, diabetes, organ transplantati

266 could be responsible for mediating systemic immunosuppression that antagonizes anti-PD-1 checkpoint

267 ation and chronic inflammatory disease cause immunosuppression that can be difficult to reverse.

268 w-up visits 2 and 3 years after cessation of immunosuppression, the patient exhibited normal graft fu

269 in the kidneys of healthy people, but during immunosuppression, the virus can reactivate and cause pr

270 ansplant patients have been able to decrease immunosuppression, this is the first instance of true op

271 hese data demonstrate a mechanism of TGFbeta immunosuppression through inhibition of CXCR3 in CD8(+)

272 Abrogating LAIR1 immunosuppression through LAIR2 overexpression or SHP-1

273 esponse sensor, PERK, enhances MDSC-mediated immunosuppression through the NRF2 transcription factor,

274 g regimens, in parallel with more aggressive immunosuppression to better control graft-versus-host di

275 rgical procedure, and the pathophysiology of immunosuppression to ensure optimal outcomes.

276 e with belatacept did not provide sufficient immunosuppression to reliably prevent pancreas rejection

277 ery of a nationalized database for VCA type, immunosuppression treatment, and clinical outcomes for V

278 eaths and rejections, compared with standard immunosuppression tritherapy.

279 ion is limited by adverse effects of chronic immunosuppression used to control rejection.

280 Immunosuppression was associated with 6-fold greater odd

281 Immunosuppression was based on CNI (tacrolimus), steroid

282 All immunosuppression was discontinued on postoperative day

283 may be more widely performed if maintenance immunosuppression was not essential for graft acceptance

284 gical disease models, we determined that the immunosuppression was not unique to cancer itself, but r

285 ld be increased in patients in whom relative immunosuppression was the major feature of their sepsis

286 To stop TAM-mediated immunosuppression, we use a novel treatment by injecting

287 mycophenolate mofetil-tacrolimus maintenance immunosuppression were analyzed.

288 Multiple features of potential immunosuppression were observed, including T regulatory

289 Both thymic involution and serum-derived immunosuppression were reversible upon clearance of brai

290 Baseline characteristics and maintenance immunosuppression were similar.

291 esults suggest that hypoxic exposure induces immunosuppression which could increase vulnerability to

292 reveal a powerful mechanism of HPV-mediated immunosuppression, which can be exploited to improve res

293 (TAMs) mediate angiogenesis, metastasis, and immunosuppression, which inhibits infiltration of tumor-

294 Both groups received immunosuppression with cyclosporin A and everolimus in t

295 ar disease (HR, 2.19; 95% CI, 1.2-3.98), and immunosuppression with cyclosporine A (HR, 1.93; 95% CI,

296 Sepsis causes inflammation-induced immunosuppression with lymphopenia and alterations of CD

297 ned graft survival in the absence of chronic immunosuppression with potential clinical implications.

298 t the time of a screening biopsy to enter an immunosuppression withdrawal trial.

299 ney model, the liver was rejected soon after immunosuppression withdrawal.

300 or cells (MDSCs) are immune cells that exert immunosuppression within the tumor, protecting cancer ce