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1 EMD + NBM-treated defects showed a mean CAL change from
2 EMD 57033-binding protects myosin against heat stress an
3 EMD also enhanced (by 20% to 40%) the expression of tran
4 EMD and P2 promoted reepithelialization and neovasculari
5 EMD and P2 significantly promoted early wound closure at
6 EMD exhibited strong cytotoxicity toward various human l
7 EMD gel adsorbed less protein to the surface of grafting
8 EMD had an effect on levels of cytokines related to fibr
9 EMD had no effect on the epithelial gap of the wound.
10 EMD improves oral mucosa incisional wound healing by pro
11 EMD induced a concentration-dependent increase of CTGF p
12 EMD induced dramatic c-Myc degradation through a ubiquit
13 EMD maintained a significant acceleration of reepithelia
14 EMD may provide greater DF compared to non-treated contr
15 EMD may provide greater DF under diabetic or normal cond
16 EMD or TGF-beta1 provoked a significant increase of IL-1
17 EMD provided an increased defect fill (DF) in G1 and hig
18 EMD provided an increased DF in both groups and enhanced
19 EMD provides highest levels of CRC; however, the additio
20 EMD significantly increased cell proliferation at 3 and
21 EMD significantly increased PMN chemotactic activity (P
22 EMD stimulates CTGF expression in human PDL cells, a pro
23 EMD therapy of intrabony defects promotes additional ben
24 EMD treatment predictably alters a dysbiotic subgingival
25 EMD+CAF continues to show histologic evidence of periodo
26 EMD- and TGF-beta1-stimulated CTGF expression was signif
29 Mutations in LMNA encoding lamin A/C and EMD encoding emerin cause cardiomyopathy and muscular dy
34 that the combination of EMD liquid + NBM and EMD liquid + DFDBA adsorbed higher amounts of amelogenin
38 In univariable analysis, the presence of any EMD ( P = .005), skin involvement ( P = .002), spleen (
40 ur, which was similar to adjacent tissues at EMD-treated sites but greater than adjacent tissues at a
44 ng the frequency of CAL gain >/=4 mm between EMD + DBBM (60%) and CM + DBBM (50%) or comparing the fr
48 urthermore, amelogenin proteins delivered by EMD liquid were able to penetrate the porous surface str
50 ver, the anti-inflammatory effect induced by EMD observed in the in vitro study could not be confirme
51 f the epithelial barrier function induced by EMD were investigated by analysis of transepithelial ele
57 superior length of NC [4.13 +/- 1.22 (CAF + EMD); 3.95 +/- 1.11 (CAF + CM + EMD); 2.94 +/- 0.77 (CAF
58 with the other groups [1.09 +/- 0.26 (CAF + EMD); 1.04 +/- 0.34 (CAF + CM); and 1.14 +/- 0.29 (CAF),
59 0.68 (CAF + CM + EMD); 3.01 +/- 0.56 (CAF + EMD); 2.15 +/- 0.47 (CAF + CM); 2.29 +/- 0.82 (CAF), P =
71 A superior STT was observed for CAF + CM + EMD group (1.5 +/- 0.33) when compared with the other gr
72 1.22 (CAF + EMD); 3.95 +/- 1.11 (CAF + CM + EMD); 2.94 +/- 0.77 (CAF + CM); 2.72 +/- 0.81 (CAF), P =
73 P = 0.02] and NB [3.21 +/- 0.68 (CAF + CM + EMD); 3.01 +/- 0.56 (CAF + EMD); 2.15 +/- 0.47 (CAF + CM
76 results of this study suggest that combining EMD and SPPF in the treatment of suprabony defects may l
78 ial than the commercially available complete EMD compound and that the mechanism of action, in part,
80 Six of these pools, along with the complete EMD unfractionated compound and positive and negative co
84 ups during follow-up (P <= 0.05), and AgP+CS/EMD presented a higher rCAL gain (2.4 +/- 1.0 mm) when c
88 of young adults-the Eccentric Muscle Damage (EMD; n = 156) cohort and the Functional Single Nucleotid
91 cal application of enamel matrix derivative (EMD) added to papilla reflection/root preparation (PR/RP
93 the combination of enamel matrix derivative (EMD) and natural bone mineral (NBM) with and without add
95 ue graft (CTG) and enamel matrix derivative (EMD) approaches provided superior initial REC reduction
96 effect of using an enamel matrix derivative (EMD) as an adjunct to non-surgical periodontal therapy (
97 are the effects of enamel matrix derivative (EMD) associated with a hydroxyapatite and beta-tricalciu
98 e effectiveness of enamel matrix derivative (EMD) associated with a simplified papilla preservation f
99 en matrix (CM) and enamel matrix derivative (EMD) characteristics, it is suggested that their combina
101 matrix (CM) and/or enamel matrix derivative (EMD) for the treatment of dehiscence-type recession defe
103 eriodontal therapy enamel matrix derivative (EMD) has been successfully used for tissue regeneration
107 matrix (CM) and/or enamel matrix derivative (EMD) in combination with a coronally advanced flap (CAF)
108 ix graft (ADMG) or enamel matrix derivative (EMD) in conjunction with a coronally advanced flap (CAF)
109 ) with and without enamel matrix derivative (EMD) in the treatment of multiple Class III-IV Miller pe
111 entered results of enamel matrix derivative (EMD) therapy in intrabony defects in aggressive periodon
113 the association of enamel matrix derivative (EMD) with ABG in the management of intrabony defects (IB
114 regeneration (GTR)/enamel matrix derivative (EMD) with and without laser treatment, the WMD of PD was
115 t a combination of enamel matrix derivative (EMD) with demineralized freeze-dried bone allograft (DFD
116 on treatments with enamel matrix derivative (EMD), a commercial formulation of EMPs, suggest that it
117 uate the effect of enamel matrix derivative (EMD), tyrosine-rich amelogenin peptide (TRAP), and a syn
118 ed with an enamel matrix protein derivative (EMD) combined with either a natural bone mineral (NBM) o
125 estrous phases (estrus/metaestrus/diestrus (EMD)) froze more during extinction retrieval than those
128 10 years and between treatment groups (i.e., EMD versus CTG) at the same time points were examined.
130 ent study, regenerative therapy using either EMD + DBBM or CM + DBBM yielded comparable clinical outc
131 one grafts after surface coating with either EMD (as a liquid formulation) or EMD (as a gel formulati
132 llow-up investigation, treatment with either EMD + CAF or CTG + CAF for Miller Class I and II GR defe
133 ndomly assigned to the treatment with either EMD + DBBM (test: n = 20) or CM + DBBM (control: n = 20)
138 f the defects amounted to 6.1 +/- 1.9 mm for EMD + DBBM and 6.0 +/- 1.9 mm for CM + DBBM sites (P = 0
139 he potential for a liquid carrier system for EMD, used to coat EMD, may be advantageous for better su
140 lonal antibody was loaded onto the Fractogel EMD SO3 (M) cation exchanger at either pH 5 or pH 4.
144 e WMD of PD was negligible; however, the GTR/EMD group showed better outcomes (P = 0.005) than the la
145 e Department of Muhimbili National Hospital (EMD-MNH) in Dar Es Salaam, Tanzania with non-traumatic a
148 11 clinical trials, were studied to identify EMD, as defined by physical examination, laboratory find
149 en freezing and IL-BLA circuit activation in EMD animals, and a negative correlation in PRO animals.
154 ning of 5'SS-branchpoint length in our index EMD case subject defines 45-47 nt as the critical elonga
156 ertebrate visual cortex the output from many EMDs is pooled in neurons sensitive to wide-field optic
159 N-bis (5-ethyl-2-hydroxybenzyl) methylamine (EMD), and present evidence demonstrating its effectivene
160 N-bis (5-ethyl-2-hydroxybenzyl) methylamine (EMD), in targeting c-Myc in several lung cancer cell lin
167 aim of this study is to test the ability of EMD to adsorb to the surface of DFDBA particles and dete
168 anticancer and c-Myc-targeted activities of EMD support its use in potential new approaches to treat
169 beta receptor I kinase-dependent activity of EMD and make it available for potential target cells.
172 The results suggest that the addition of EMD to DFDBA particles may influence periodontal regener
174 d controversial results after application of EMD combined with different types of bone grafting mater
176 efects after treatment with a combination of EMD and biphasic calcium phosphate (BC) or EMD alone.
177 n assay demonstrated that the combination of EMD liquid + NBM and EMD liquid + DFDBA adsorbed higher
178 ith this information, selected components of EMD can now be formulated for optimal osteo- and angio-g
180 e present study was to compare the effect of EMD and its fractions on the cytokine profiles from huma
181 DFDBA particles and determine the effect of EMD coating on downstream cellular pathways such as adhe
184 This study examines the in vivo effects of EMD on healing of an oral mucosa surgical wound in rats.
185 igate proliferative and cytotoxic effects of EMD on oral epithelial cells and their possible influenc
193 risk and WBC count, neither the presence of EMD nor the number of specific sites of EMD were indepen
195 Most patients (65.3%) had only one site of EMD, 20.9% had two sites, 9.5% had three sites, and 3.4%
197 , in certain clinical situations, the use of EMD alone may not be sufficient to prevent flap collapse
206 s provide the best outcomes, whereas ADMG or EMD in conjunction with CAF may be used as an alternativ
215 with regenerative surgery using EMD + NBM or EMD + beta-TCP can be maintained over a period of 10 yea
221 PPF technique; 25 participants also received EMD (test group) and 25 patients underwent flap surgery
222 ler Class I and II GR, each patient received EMD+CAF for three teeth and CTG+CAF for one tooth for ro
224 roximal PD were randomly allocated to (PR/RP+EMD; n = 24) and control (PR/RP+saline; n = 26) therapie
227 ness flaps were raised, and, after suturing, EMD was injected underneath the soft tissues on one side
230 onclusion This large study demonstrates that EMD at any site is common but is not an independent prog
231 e results of the present study indicate that EMD application, irrespective of the combination with CM
232 Cycloheximide chase assay revealed that EMD tended to shorten the half-life of c-Myc by approxim
242 ed an RMSE of 7.3 days, a PC of 0.93 and the EMD ranged between -6.4 and 4.1 days while the conventio
245 4% (i.e., seven of 11) of the defects in the EMD + NBM group and in 82% (i.e., nine of 11) of the def
251 s from baseline values, including wKT in the EMD group, which at 1 year was not significantly improve
253 CAL gain of 2.38 +/- 2.17 mm (24.9%) in the EMD/BC group and 2.65 +/- 2.18 mm (36.2%) in the EMD gro
254 eductions of 3.14 +/- 1.95 mm (39.6%) in the EMD/BC group and 3.30 +/- 1.89 mm (48.7%) in the EMD gro
255 At 12 and 24 months after treatment, the EMD + HA/beta-TCP group showed significantly greater PD
256 th the soft tissues on one side, whereas the EMD vehicle was injected in the contralateral side.
258 nd in vivo, the specific elements within the EMD compound responsible for these effects remain unknow
262 ) were found for SCTG + CAF when compared to EMD + CAF (MD: -1.06 mm), and SCTG + CAF when compared t
264 available collagen products were exposed to EMD or recombinant TGF-beta1, followed by vigorous washi
265 ricalcium phosphate (HA/beta-TCP) implant to EMD alone and to open-flap debridement (OFD) when surgic
266 n matrix to adsorb the activity intrinsic to EMD that provokes transforming growth factor (TGF)-beta
267 nts obtained with regenerative surgery using EMD + NBM or EMD + beta-TCP can be maintained over a per
268 lity of the gingival margin over time, while EMD, acellular dermal matrix, collagen matrix, and flap
271 osed, using a bone graft in combination with EMD to avoid collapse of the flap into the bony defect d
272 ment of non-contained infrabony defects with EMD, with or without BC, resulted in statistically signi
274 nct of an HA/beta-TCP composite implant with EMD may improve the clinical and radiographic outcomes o
281 cles were precoated in various settings with EMD or human blood and analyzed for protein adsorption p
284 The mean CAL gain at sites treated with EMD + DBBM was not statistically significantly different
285 n 83% (10 of 12) of the defects treated with EMD + NBM + PRP and in 100% (all 12) of the defects trea
289 imary keratinocytes were either treated with EMD dissolved in culture medium or added to wells/insert
299 ar-weight protein pools (7 to 17 kDa) within EMD have greater osteoinductive potential than the comme
300 ling and root planing (SRP) with and without EMD in 51 patients presenting with moderate to severe pe