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1 conjugated estrogen; r = -0.507, P=0.004 for combined therapy).
2 Lactococcus lactis as tolerogenic adjuvant (combined therapy).
3 blockade, prompting a follow-up trial of the combined therapy.
4 ation, which were further enhanced following combined therapy.
5 treated at some point with either single or combined therapy.
6 d highlights the clinical potential for this combined therapy.
7 moral tissue was still intact 24 h after the combined therapy.
8 im analysis revealed significant benefit for combined therapy.
9 herapy for stable or responding patients was combined therapy.
10 ich PAKs mediate resistance to BRAFi and the combined therapy.
11 hereas there was no effect with IV vitamin C combined therapy.
12 tments further augmented the efficacy of the combined therapy.
13 rlie acquired resistance to BRAFi and to the combined therapy.
14 lease of cargoes to achieve multi-functional combined therapy.
15 utcome was to assess the long-term safety of combined therapy.
16 he realistic application of phage-antibiotic combined therapy.
17 CGT level in tumors subjected to CGT-NP+UTMD combined therapy.
18 otic and autophagy activities induced by the combined therapy.
19 s of contextualization, optimal arousal, and combined therapy.
20 ventricular size and function in response to combined therapy.
21 tion abrogated the therapeutic effect of the combined therapy.
22 nt was eradication of MRD after 12 months of combined therapy.
23 sify therapy, switch to another drug, or use combined therapy.
24 of tamoxifen response and personalisation of combined therapies.
25 tial clinical and immunologic effects of the combined therapies.
26 , it was less common in the groups receiving combined therapy (34/130 [26%]) than in the group treate
27 ng: tracer-determined glucose disposal rate (combined therapy, 52.4 +/- 2.9 mg x kg(-1) x min(-1), vs
28 te grade 3 mucositis was more prevalent with combined therapy, 84% v 43% (P <.001), resulting in a hi
29 lone, as compared with patients who received combined therapy (95 percent confidence interval, 1.10 t
31 of renal interstitial fibrosis; therefore, a combined therapy aimed at simultaneously targeting multi
32 alysis of pulmonary metastases revealed that combined therapy also had a more potent antimetastatic e
37 2.4 +/- 0.4 (standard error of the mean) for combined therapy and 0.9 +/- 0.2 for RF ablation alone (
38 was 49.0 months among patients treated with combined therapy and 29.3 months among those treated wit
40 o significant differences were found between combined therapy and ligation in rebleeding (29% vs. 30%
41 indings highlight an additive benefit of the combined therapy and potential new unique roles of utrop
42 cterize pathophysiological changes following combined therapy and to determine whether radioresponse
44 increases in the immune responses (from the combined therapy) and duration of antibody response that
45 , 1 patient died suddenly while treated with combined therapy, and 1 patient died of unrelated causes
46 nts had resuscitated cardiac arrest while on combined therapy, and 1 patient had repeated, appropriat
47 i67 proliferation index were documented with combined therapy, and EGFR down-regulation was observed
48 jor treatments were no therapy, monotherapy, combined therapy, and potent antiretroviral therapy, res
49 eing treated with methotrexate-sulfasalazine combined therapy, and two of the patients were being tre
50 beta-blocker therapy and continuous pacing, combined therapy appears to provide reasonable, long-ter
52 rogression-free survival was improved in the combined therapy arm (median not reached) compared with
54 of disease and intermittent hormone therapy (combined therapy arm; n = 43) or to hormone therapy only
56 ial resistant strains, support the design of combined therapy, as well as assist the development of t
59 ow that treatment of C57BL/6 donor mice with combined therapy before the transplant protects the reci
61 replicon particles (HPV16-VRP) and that this combined therapy can eradicate human papillomavirus 16 (
62 t demonstrates that orthodontic-regenerative combined therapy can resolve complex clinical problems a
64 noma of the prostate, but outcome using this combined therapy compared with RT alone is not known.
65 duced microvessel counts in the tumors given combined therapy compared with the tumors given either a
67 diopathic long-QT syndrome were treated with combined therapy consisting of continuous cardiac pacing
70 ptimal dose of anti-CD3 monoclonal antibody (combined therapy [CT], 1 x 5 mug [CT5]) reverts diabetes
71 ptimal dose of anti-CD3 monoclonal antibody (combined therapy [CT], 1 x 5 ug [CT5]) reverts diabetes
72 oup as a whole; however, in 50% of patients, combined therapy decreased PVRI by 20% more than did iNO
73 Surprisingly, the animals treated with the combined therapy did not perform as well as postnatally-
74 deletion of CD20-bearing cells and that the combined therapy did not significantly impair establishe
77 , 250 microL; total dose, 0.5 mg) alone; (c) combined therapy (doxorubicin injection immediately foll
82 d dose (480 mg/m(2)), five patients received combined therapy first and carboplatin alone second, and
88 , and topical growth factors, referred to as combined therapy, for treating hypertrophic scars compar
89 eaths from non-small-cell lung cancer in the combined therapy group (62 vs 31 deaths; 0.09%vs 0.05%;
90 ity (BCVA) improved from 0.73 to 0.53 in the combined therapy group (P < .001) and from 0.79 to 0.72
91 istically significant after 21 months in the combined therapy group and 15 months in the monotherapy
92 mothermia (p < 0.01) (although >40mmHg); the combined therapy group required more fluid boluses (p <
93 achment, whose TNFalpha concentration in the combined therapy group was the lowest value found (53.50
96 te of overall survival was 55 percent in the combined-therapy group and 34 percent in the hyperfracti
97 years were 67 percent among patients in the combined-therapy group and 40 percent among patients in
98 The median survival was 72.2 months in the combined-therapy group and 59.3 months in the monotherap
99 e occurred in 113 participants (3.6%) in the combined-therapy group and in 157 (5.0%) in the dual-pla
101 ciliter (0.87 mmol per liter) greater in the combined-therapy group than in the dual-placebo group, a
102 akness and dizziness were more common in the combined-therapy group than in the dual-placebo group, b
103 onal control was significantly higher in the combined-therapy group than in the group given radiother
104 ree survival was significantly longer in the combined-therapy group than in the radiotherapy group (h
107 eiving radiotherapy plus short-term ADT (the combined-therapy group), as compared with 57% among pati
108 l and regional control was 82 percent in the combined-therapy group, as compared with 72 percent in t
116 ized freeze-dried bone (DFDB) grafting (BG), combined therapy (GTR + BG) and a DFDB-glycoprotein spon
121 This fully oral, chemotherapy-free, triplet combined therapy has the potential to be an alternative
125 s lesions, supporting the potential of these combined therapies in the treatment of advanced atherosc
126 out toxicity, showing the potential of these combined therapies in the treatment of advanced atherosc
127 rt demonstrates orthodontic and regenerative combined therapy in a 49-year-old male whose right maxil
129 podia regulation that points to the need for combined therapy in order to prevent invadopodia-mediate
130 s to summarize our long-term experience with combined therapy in patients with long-QT syndrome.
132 possibility that both agents can be used as combined therapy in the treatment of ischemic heart dise
133 and decreased during both lisinopril and the combined therapy in which it was not different from base
136 In comparison with individual treatments, combined therapy (iNO + dipyridamole) did not augment pu
138 utic responses are T-cell-dependent, because combined therapy is not efficacious in severe combined i
139 observed in DMD patients, the effect of the combined therapy is slightly attenuated but still benefi
140 t of the widespread clinical impression that combined therapy is superior to psychotherapy alone for
141 al role played by PRP, BPBM, and GTR in this combined therapy is unclear and needs to be elucidated.
146 at 84 weeks and 2 participants receiving all combined therapies maintained viral loads below 1000 cop
147 ng on a decision maker's willingness to pay, combined therapy may be cost-effective, particularly for
149 effective only as long as they are used, and combined therapy may be more effective than monotherapy.
152 and glucocorticoids plus rituximab were the combined therapies most frequently employed during remis
153 injected liposomal doxorubicin (n = 26), or combined therapy (n = 30) and were compared with control
157 tudy, we present seven patients for whom the combined therapies of PP/IVIG were successful in reversi
158 pes or pulsed-HIFU exposure in addition to a combined therapy of (90)Y-B3 and taxol to enhance the sy
160 s stages of prostate cancer cells and that a combined therapy of antiandrogens and anti-PI3K/Akt inhi
161 e increased to 5.98 (95% CI, 0.72-216.0) for combined therapy of atorvastatin, pravastatin, or simvas
167 findings suggest consideration of applying a combined therapy of GLS inhibitor and PARP inhibitor to
168 rpose of this study was to determine whether combined therapy of glutaraldehyde-polymerized bovine he
173 icroL of ethanol infused over 1 minute); (c) combined therapy of PEI immediately followed by RF ablat
175 immediately followed by RF ablation; or (d) combined therapy of RF ablation immediately followed by
177 BMP7 and LfcinB as individual treatments and combined therapy on bovine nucleus pulposus (NP) cells b
178 n are added to statin therapy, the effect of combined therapy on LDL cholesterol levels is additive.
181 d for selecting patients for more aggressive combined therapies or enrollment into trials targeting E
182 engineered into multispecific constructs for combined therapies or for use in new strategies such as
184 of lifestyle-modification counseling (i.e., combined therapy); or sibutramine plus brief lifestyle-m
187 change in PAI-1 during ramipril (P=0.011) or combined therapy (P=0.006) but not during estrogens (P=0
190 Model-predicted cellular responses to the combined therapy provide good agreement with experimenta
194 and abandonment of treatment modalities and combined therapy regimens were examined overall, by coun
210 ttempted, but the effects of augmentation on combined therapies, such as cognitive remediation and so
211 as paved the way to consider refinements and combined therapies, such as the use of biomaterials to a
212 mouse model of autoimmune diabetes, we show combined therapy supports regulatory T cell homeostasis
214 phages manifested an M2-like profile(3), the combined therapy synergistically enhanced antitumour eff
218 neuroprotective activities, suggesting that combined therapies targeting distinct Ass42 epitopes can
220 nhibitors, by targeted ER degradation, or by combined therapy targeting both ER and growth factor sig
221 pport a personalized medicine approach where combined therapy targeting YAP and Bcl-2, tailored to NF
223 te of response was significantly higher with combined therapy than with placebo (79.2 percent vs. 54.
224 dentify new therapeutic targets, and lead to combined therapies that are effective against highly het
225 ical evidence-based adjunctive therapies and combined therapies that can be used to tailor individual
226 oenvironmental impacts, and discuss targeted/combined therapies to overcome immune evasion and the bi
228 lenge current trial design paradigm that for combined therapy to be successful individual agents shou
229 The unprecedented capacity of this novel combined therapy to eliminate amyloid deposits should be
231 s to lie in a multidimensional approach with combined therapy to manage both cancer cachexia and asth
232 preclinical data supporting the use of this combined therapy to overcome the limitations of standard
233 ify LDLR as a promising metabolic target for combined therapy, to limit PDAC progression and disease
235 t different sites and may help us to develop combined therapies using anti-AR and anti-VEGF-C compoun
236 rogramming CAFs and provides a rationale for combined therapies using inhibitors of AKT and CX3CR1.
239 85% of patients (39 of 46) in group A given combined therapy versus 11% (5 of 46) receiving lamivudi
240 rred in 31% of patients (14 of 45) receiving combined therapy versus 6% (3 of 48) receiving lamivudin
242 widths were also significantly greater with combined therapy versus PF alone (8.6+/-1.8 mm radiofreq
244 years of follow-up the overall survival for combined therapy was 26% (95% confidence interval [CI],
245 The 6-month maintenance response rate for combined therapy was 57.1% for the PDSS (P=.04 vs CBT al
249 A and SAMe treatment prevented this fall and combined therapy was more effective on preserving GSH le
255 s (56 underwent monotherapy and 72 underwent combined therapy), which were followed-up for up to 15 m
256 dge, and argue that significant progress for combined therapies will require a better understanding o
257 roaches as well as their potential to obtain combined therapies with desired drug release profiles.
258 b, adalimumab, certolizumab, vedolizumab, or combined therapies with placebo or an active agent for i
259 2139 once per week for 15 weeks, followed by combined therapy with 250 mg intravenous REP 2139 and 18
264 14 trial, a dose-ranging angiographic study, combined therapy with abciximab plus reduced-dose tPA en
267 ment of HER-positive breast cancer, although combined therapy with anthracycline-based regimens has b
271 nscheduled DNA synthesis that was reduced by combined therapy with antireceptor antibody specific to
275 l hemodynamic response to traditional NSBBs, combined therapy with carvedilol plus simvastatin signif
280 tained with the combination, suggesting that combined therapy with IGF-1 and OP-1 may be an effective
281 vidence in this study strongly suggests that combined therapy with inhibitors of YAP (such as vertepo
282 o treatment demonstrates a possible role for combined therapy with iNO and PGI2 in infants with sever
284 PTEN/PI3K pathway that would be amenable to combined therapy with MAPK pathway inhibitors for the tr
286 l was conducted to determine the efficacy of combined therapy with olanzapine and either valproate or
288 patients with C4d positive AHR who received combined therapy with PPH and polyclonal rabbit antithym
290 ctivator (rtPA) makes it a candidate for the combined therapy with rtPA for the acute treatment of is
296 e compared the 3180 participants assigned to combined therapy (with rosuvastatin and the two antihype