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1 SAP colocalized with SLAMF6 only in association with clu
2 SAP consisted of single-shot, intravenous infusion of 1.
3 SAP domains are common among many other SUMO E3s, and ar
4 SAP expression is required for the counterselection of d
5 SAP functions are mediated, in part, by FcgammaRs, but t
6 SAP in the first 14 days was diagnosed by a criteria-bas
7 SAP mediates this function by coupling SLAM family recep
8 SAP performed significantly better than FDT in predictin
9 SAP, SLP, and OCT outcomes were compared between the con
10 Interestingly, in the presence of Ca(2+), SAP first inhibited, then significantly accelerated D76N
14 a under the curve, 0.81; 95% CI, 0.72-0.90), SAP mean sensitivity (area under the curve, 0.80; 95% CI
15 ation increased after TCR restimulation in a SAP-dependent manner, requiring both immunoreceptor tyro
16 recombinase-mediated gene deletion to ablate SAP expression after completion of iNKT cell development
19 Carriers with SH2D1A mutations abolishing SAP expression and low percentage of SAP(+) cells showed
20 d to construct expression vectors to achieve SAP overexpression, and both genetic and functional assa
25 reaction times even after adjusting for age, SAP mean deviation in the better eye, cognitive ability,
27 urve, 0.80; 95% CI, 0.69-0.88; P = .03), and SAP pattern standard deviation (area under the curve, 0.
32 numbers of apoptotic cells, stronger C4d and SAP deposition, and extensive activated caspase 3 were f
34 present on mouse lung epithelial cells, and SAP and the aminothiazole potentiate IL-10 production fr
40 d healthy controls were examined by FDT2 and SAP, both with the 24-2 test pattern, on the same day at
41 ey aspects of inflammation and fibrosis, and SAP injections improve lung function in pulmonary fibros
44 n of radiolabelled peptide p5+14 with p5 and SAP, in amyloid-laden mice, using dual-energy SPECT imag
45 the presence of concentrations of serum and SAP that normally completely inhibit fibrocyte different
48 Treatment with CPHPC followed by an anti-SAP antibody safely triggered clearance of amyloid depos
55 a key paracrine factor of BMSCs attenuating SAP targeting the NF-kappaB1/p50 gene and suppressing th
58 Each 1 decibel (dB)/year change in binocular SAP MS was associated with a change of 2.0 units in the
59 ty index, each 1 dB/year change in binocular SAP MS was associated with a change of 3.0 units in the
60 severity and the rate of change in binocular SAP sensitivity, each 1-mum-per-year loss of RNFL thickn
65 ls in patients with XLP seem functional, but SAP-deficient T cells were resistant to Treg cell-mediat
68 thickness change in eyes that progressed by SAP were faster than in those that did not progress (-1.
72 ter first using CPHPC to deplete circulating SAP, we infused a fully humanized monoclonal IgG1 anti-S
73 (conA), and human serum amyloid P component (SAP) at elevated temperatures prior, during, and after d
74 protein (CRP) and serum amyloid P component (SAP), two major classical pentraxins in humans, are solu
79 values below the range of healthy controls (SAP(dull)), and 1, carrying the R55L mutation, was SAP(+
81 carboxylic acid (CPHPC) efficiently depletes SAP from the plasma but leaves some SAP in amyloid depos
84 ate of FDT PSD change in eyes that developed SAP visual field loss was 0.07 dB/year versus 0.02 dB/ye
85 algorithm-defined versus physician-diagnosed SAP in 1088 patients who had dysphagic acute stroke from
89 tients examined for glaucoma and to evaluate SAP, OCT and RGC counts capability to discriminate the w
96 5% CI, 0.86-0.96), which was larger than for SAP mean deviation (area under the curve, 0.81; 95% CI,
97 antibodies isolated from single B cells from SAP-deficient patients with X-linked lymphoproliferative
98 After adjusting for the contribution from SAP, 26% (95% CI, 12%-39%) of the variability of change
99 baseline and rate of change information from SAP had stronger ability to predict change in NEI VFQ-25
101 iferative disease (XLP), who lack functional SAP, were hyperresponsive to PD-1 signaling, confirming
107 lesions of the MSDB using GAT1-saporin (GAT1-SAP) and examined on spontaneous exploration (Experiment
109 However, the precise cellular basis of how SAP deficiency contributes to immune dysfunction remains
114 gulation of central tolerance, we identified SAP expression in a discrete subset of bone marrow immat
118 fied functionally significant amino acids in SAP form a binding site that is distinct from the previo
120 r subjects with the same amount of change in SAP sensitivity, those with shorter follow-up times had
122 corrects the cellular and humoral defects in SAP(-/-) mice providing proof of concept for gene therap
123 r arbitrary values of intereye difference in SAP mean deviation (MD) of 0, 5, 10, and 15 dB were 0.58
125 evaluated the role of pancreatic lipases in SAP-associated visceral fat necrosis, the inflammatory r
127 uced similar anti-RABV antibody responses in SAP-deficient and wild-type mice, demonstrating that BAF
128 germinal center formation, were restored in SAP-transduced mice.We demonstrate for the first time th
131 tic fat lipolysis plays an important role in SAP, we evaluated the role of pancreatic lipases in SAP-
132 LCBI and the primary endpoint was similar in SAP and ACS patients (p value for heterogeneity = 0.14).
133 mum set of items that should be addressed in SAPs for clinical trials, developed with input from stat
135 o a complete ophthalmic evaluation including SAP and Spectral Domain OCT (SD-OCT) of RNFL and macular
142 ormed in Europe by using iodine-123-labelled SAP; however, this tracer is not available in the US.
143 y, we found that CD4 and CD8 T cells lacking SAP had a diminished capacity to differentiate into IL-1
145 odel adjusting for baseline MoCA score, mean SAP MD, age, sex, race/ethnicity, educational level, inc
148 isual field was estimated from the monocular SAP tests, and rates of change in mean sensitivity (MS)
152 he pro- and anti-amyloidogenic activities of SAP are not mutually exclusive, but reflect two sides of
157 OR of algorithmic and physician diagnosis of SAP were assessed using adjudicated SAP as the reference
161 necrosis volume of 112.5 ml was a marker of SAP and 433.0 ml cut-off value could be used to predict
163 n hepatic amyloid load, as shown by means of SAP scintigraphy and measurement of extracellular volume
167 ty, educational level, income, and number of SAP tests, each 5-point decline in MoCA score was associ
168 lishing SAP expression and low percentage of SAP(+) cells showed neutral 2B4 function at the polyclon
178 , with a lower dose of collagen, the role of SAP was more dependent on Fyn binding, suggesting that a
183 gest that the physiological contributions of SAPs to vaginal immunopathology require hypha formation,
185 uencing (NGS) data and the identification of SAPs through database searching, post-processing and gen
188 dict the development of visual field loss on SAP, adjusting for confounding variables (baseline age,
191 rombin may be an initial trigger to override SAP inhibition of fibrocyte differentiation to initiate
192 lated human serum proteins, serum amyloid P (SAP) and C-reactive protein (CRP), strongly affect fibro
193 lylated glycoprotein called serum amyloid P (SAP) inhibits fibrocyte differentiation, and sialidases
195 bited by the plasma protein serum amyloid P (SAP), and healthy tissues contain very few fibrocytes.
196 ith the fibrocyte inhibitor serum amyloid P (SAP; pentraxin-2) significantly prolonged survival and s
197 n associated with severe acute pancreatitis (SAP) for over 100 years; however, its pathogenesis and r
199 m tuberculosis sulfate-assimilation pathway (SAP) represent major immunogenic targets of the bacillus
200 linked lymphoproliferative disease patients, SAP deficiency reduces CD74 expression, resulting in the
201 graphy for suspected stable angina pectoris (SAP) (n = 4131) and an independent cohort of patients wh
204 ity indices in standard automated perimetry (SAP) affect the global indices of visual field (VF) resu
205 monitored with standard automated perimetry (SAP) and had longitudinal assessment of cognitive abilit
206 l subjects had standard automated perimetry (SAP) and optical coherence tomography was used to measur
207 re tested with standard automated perimetry (SAP) at 6-month intervals, and evaluation of rates of vi
211 table abnormal standard automated perimetry (SAP) or progressive glaucomatous changes on stereophotog
212 t one reliable standard automated perimetry (SAP) test, while RNFL measurements were obtained using t
213 eld loss using standard automated perimetry (SAP) when considering different frequencies of testing u
215 be observed by Standard Automated Perimetry (SAP), the second by Optic Coherence Tomography (OCT) tha
219 atio (C/N ratio), soil available phosphorus (SAP), soil NH4(+)-N, soil NO3(-)N, aboveground biomass (
221 nths of AP use from dinner to waking up plus SAP use during the day versus 2 months of SAP use only u
222 Diagnosing stroke-associated pneumonia (SAP) is challenging and may result in inappropriate anti
223 ces the risk of stroke-associated pneumonia (SAP), or of how quickly it should be done after admissio
225 ncluding 510 single amino acid polymorphism (SAP) peptides, 2 INDEL peptides, 49 splice junction pept
226 n result in single amino acid polymorphisms (SAPs), leading to alteration of the corresponding amino
228 act of three different set anode potentials (SAPs; -0.25, 0, and 0.25 V vs. standard hydrogen electro
229 em, and the symptom association probability (SAP) test might distinguish extraesophageal manifestatio
230 We describe a spike adjustment procedure (SAP) that, unlike commonly used normalization methods in
231 ation of surgical antimicrobial prophylaxis (SAP) for the prevention of surgical site infection (SSI)
232 isplay reduced levels of the adaptor protein SAP, probably as a result of continuous T cell activatio
233 ytic activation molecule-associated protein (SAP) adaptor are important in the development of several
235 n the gene encoding SLAM-associated protein (SAP) and leads to abnormalities of NKT-cell development,
236 ytic activation molecule-associated protein (SAP) are highly susceptible to one specific viral pathog
237 tivation molecule (SLAM)-associated protein (SAP) can mediate the function of SLAM molecules, which h
241 ytic activation molecule-associated protein (SAP) was functionally and mechanistically analyzed for i
243 tivation molecule (SLAM)-associated protein (SAP), the X-linked lymphoproliferative gene product.
245 -95, PSD-93, and synapse-associated protein (SAP)102 and combining electrophysiology and transmission
249 ter-generated list in a 1:1 ratio to receive SAP early in the anaesthesia room or late in the operati
251 binding of these antibodies to the residual SAP in amyloid deposits activates complement and trigger
253 ingle dose of the immunotoxin, CD45-saporin (SAP), enabled efficient (>90%) engraftment of donor cell
254 ish Kiss1 peptide was conjugated to saporin (SAP) to selectively inactivate Kiss-R1-expressing neuron
257 ollectively, these results suggest that SLAM-SAP signaling drives the differentiation and function of
258 ognizing self-antigens, suggesting that SLAM/SAP regulate B-cell receptor-mediated central tolerance.
260 depletes SAP from the plasma but leaves some SAP in amyloid deposits that can be specifically targete
262 described the discovery of sulfonylpyridine (SAP), benzothiazole (BZT), indazole (IND), and tetrahydr
263 binding domain of p65 through its C-terminal SAP-like domain in the nuclei under the condition of inf
264 degradation of propionate in all the tested SAPs was facilitated by syntrophic interactions between
267 f iNKT cell development, we demonstrate that SAP is essential for T-cell receptor (TCR)-induced iNKT
273 to bridging of the MEF2C-bound sites by the SAP domain-containing co-activator protein myocardin, an
275 hat exhibited MSMPs that occurred during the SAP (which were treated during surgery) show SS greater
276 We demonstrate that antibody blocking of the SAP-dependent 2B4 receptor is sufficient to induce XLP-l
278 cgammaRI with an IgG-blocking Ab reduces the SAP effect on fibrocyte differentiation, and ligating Fc
280 tient-managed sensor-augmented pump therapy (SAP) during the day, versus 24 h use of patient-managed
281 nt genera detected on the anode of all three SAPs based on 16S rRNA gene sequencing were Geobacter, S
283 fat by pancreatic lipases convert mild AP to SAP independent of pancreatic necrosis and the inflammat
284 noted obesity to convert mild cerulein AP to SAP with greater cytokines, unsaturated fatty acids (UFA
285 and in Phase 1 and Phase 2 clinical trials, SAP affects several aspects of the innate immune system
296 patients with FDT2, in 17% of patients with SAP, and in 3% of patients with both techniques; in cont
298 he target range was higher with AP than with SAP use: 66.7% versus 58.1% (paired difference 8.6% [95%
299 e disease or normal T cells transfected with SAP-specific small interfering RNA, consistent with RICD
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