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1 ws for bacterial invasion, which may lead to peri-implantitis.
2 ogens Pg, Pi, Tf, and Fn are associated with peri-implantitis.
3 ies do not seem to play an important role in peri-implantitis.
4  was associated with 86% fewer conditions of peri-implantitis.
5 association between titanium dissolution and peri-implantitis.
6 for studies of initiation and progression of peri-implantitis.
7 o develop a novel rat model of polymicrobial peri-implantitis.
8  implants include peri-implant mucositis and peri-implantitis.
9 f the disease to assist in the prevention of peri-implantitis.
10 rats were used for the study of experimental peri-implantitis.
11 reduced support, and 3) recurrent/refractory peri-implantitis.
12 tification of microorganisms associated with peri-implantitis.
13 cted from healthy implants and implants with peri-implantitis.
14 yromonas gingivalis (Pg), in the etiology of peri-implantitis.
15  in resolution of inflammation could prevent peri-implantitis.
16 ful in the early prevention and treatment of peri-implantitis.
17  8) 3-month supportive care for treatment of peri-implantitis.
18 up to 10% of implants must be removed due to peri-implantitis.
19 ples from healthy implants and implants with peri-implantitis.
20  may be proposed for use in the treatment of peri-implantitis.
21 nd Campylobacter rectus with the etiology of peri-implantitis.
22 suggests the association of Eubacterium with peri-implantitis.
23 transitional phase during the development of peri-implantitis.
24 ngs in soft tissue biopsies of implants with peri-implantitis.
25 ost-effectiveness of preventing and treating peri-implantitis.
26 en oral diseases: peri-implant mucositis and peri-implantitis.
27 -implant health, peri-implant mucositis, and peri-implantitis.
28 diseases, such as peri-implant mucositis and peri-implantitis.
29 atment outcomes after surgical management of peri-implantitis.
30 ated as phase I therapy for the treatment of peri-implantitis.
31 cy of different surgical approaches to treat peri-implantitis.
32 , and sclerostin as prognostic biomarkers in peri-implantitis.
33  English that applied surgeries for treating peri-implantitis.
34  applied detoxification methods for treating peri-implantitis.
35  identify potential prognostic biomarkers of peri-implantitis.
36  the other treatment modalities for managing peri-implantitis.
37 -implant status after surgical treatment for peri-implantitis.
38 dy sample included patients with and without peri-implantitis.
39 ant mucosa of both patients with and without peri-implantitis.
40 sk groups is essential to reduce the risk of peri-implantitis.
41 ss of reconstructive procedures for treating peri-implantitis.
42 -implant mucositis, or chronic periodontitis/peri-implantitis.
43 40% of the implants showed mucositis and 10% peri-implantitis.
44 of mucositis, and a 14 times greater risk of peri-implantitis.
45 risk of developing peri-implant mucositis or peri-implantitis.
46 ree main microbial consortia associated with peri-implantitis.
47 r non-surgical treatment of mild to moderate peri-implantitis.
48 ucted in consecutive patients diagnosed with peri-implantitis.
49  be further considered as risk indicators of peri-implantitis.
50 ant crowns in place, we checked for cases of peri-implantitis.
51 s a crucial role on the onset/progression of peri-implantitis.
52 ses into health, peri-implant mucositis, and peri-implantitis.
53 s in marginal bone loss, implant failure, or peri-implantitis.
54 ible, to avoid complications associated with peri-implantitis.
55 presents a new approach in the management of peri-implantitis.
56 strated benefit in mild to moderate cases of peri-implantitis.
57  variables correlated with the occurrence of peri-implantitis.
58 ne that may help explain the pathogenesis of peri-implantitis.
59 gival debridement in patients afflicted with peri-implantitis.
60  the marginal bone loss around implants with peri-implantitis.
61 ed to represent significant risk factors for peri-implantitis.
62 amic dental implants that exhibited signs of peri-implantitis.
63 epth, and defect morphology in patients with peri-implantitis.
64  the association of systemic conditions with peri-implantitis.
65 ntenance, and placement of >=2 implants) for peri-implantitis.
66  implants displayed SUP within patients with peri-implantitis.
67 n of implants and peri-implant mucositis and peri-implantitis.
68 ion in response to chronic periodontitis and peri-implantitis.
69 sk indicators for peri-implant mucositis and peri-implantitis.
70 pe-2 diabetic and non-diabetic patients with peri-implantitis.
71 cacious treatment modality for patients with peri-implantitis?
72 were identified after resective treatment of peri-implantitis: 1) peri-implant health with a reduced
73 s in seven patients were previously lost for peri-implantitis (2.2% and 4.5% at implant- and patient-
74 ucositis (3.10 mg/L, IQR 2.35, p < 0.001) or peri-implantitis (2.7 mg/L, IQR 2.53, p = 0.002) when co
75 ts of prognosis, including the following: 1) peri-implantitis; 2) etiology; 3) awareness; 4) attitude
76 of knowledge, awareness, and attitudes about peri-implantitis; 2) information provided by dentists/sp
77 cted from 164 participants (52 patients with peri-implantitis, 54 with mucositis, and 58 with healthy
78 n were frequent findings among patients with peri-implantitis (64%), and 32% reported that living wit
79 mucositis (10.8%), and 24 implants exhibited peri-implantitis (7.6%).
80 , 57 (n(implants) = 334) were diagnosed with peri-implantitis according to the established case defin
81 dents ranked biologic advances, treatment of peri-implantitis, advances in digital dentistry, develop
82 les revealed nearly complete coverage of the peri-implantitis-affected parts by the graft material.
83                                              Peri-implantitis-affected surface conditioning with citr
84  devoid of any bone particle adhesion to the peri-implantitis-affected surfaces.
85 ded clot adhesion to citric acid-conditioned peri-implantitis-affected surfaces.
86 n four patients and one in six implants have peri-implantitis after 11 years.
87                            The prevalence of peri-implantitis after 6 to 7 years was 4.7% and 3.6% wh
88 espectively, and the cumulative incidence of peri-implantitis among patients was 24.4%.
89 nd success rates as well as the incidence of peri-implantitis among patients with a history of period
90 Furthermore, the prevalence of mucositis and peri-implantitis among the study cohort was evaluated, c
91                                              Peri-implantitis, an inflammation caused by biofilm form
92      Submucosal plaque from 20 implants with peri-implantitis and 20 healthy implants was collected w
93 without MetS, where 26.3% of implants showed peri-implantitis and 55.5% mucositis.
94 nificantly reduce the reported prevalence of peri-implantitis and bring new risk factors into focus.
95 crude association between moderate to severe peri-implantitis and CVD (odds ratio = 2.18, 95% CI, 1.0
96  The associated microbiota resembles that of peri-implantitis and destructive periodontal disease in
97 oss around teeth increased the occurrence of peri-implantitis and implant loss.
98  have a poor understanding and perception of peri-implantitis and its impact.
99 s in plaque associated with ligature-induced peri-implantitis and ligature-induced periodontitis were
100 sures were implant success, implant failure (peri-implantitis and loss of osseointegration), marginal
101                          Comparisons between peri-implantitis and mucositis demonstrated significantl
102  whereas 22.5% and 56.2% were diagnosed with peri-implantitis and mucositis, respectively.
103 Again, few differences were detected between peri-implantitis and mucositis.
104 ifferential diagnoses compared with marginal peri-implantitis and other implant-related conditions.
105 ival OB of patients with type 2 diabetes and peri-implantitis and patients with peri-implantitis with
106 e odds ratios (95% confidence intervals) for peri-implantitis and peri-implant mucositis for cement-
107             Biomarker levels were similar in peri-implantitis and periodontitis groups (P >0.05).
108 ociated with the progression of experimental peri-implantitis and periodontitis induced concurrently
109 ociated with the progression of experimental peri-implantitis and periodontitis occurring concurrentl
110 t regimens may require revisions to minimize peri-implantitis and prevent bone loss.
111 ubjects presenting at least one implant with peri-implantitis and received surgical anti-infective th
112 hy peri-implant conditions and patients with peri-implantitis and to explore the influence of various
113 y is to investigate the treatment outcome of peri-implantitis and to identify factors influencing the
114 eters of subjects that have been treated for peri-implantitis and were enrolled in a regular maintena
115 tis (group A), non-diabetic individuals with peri-implantitis and without diabetes (group B), and ind
116 ble to bleeding upon probing, periodontitis, peri-implantitis, and tooth loss.
117 h (58 implants [19 healthy, 20 mucositis, 19 peri-implantitis] and 39 natural teeth [19 healthy, 12 g
118             A large number of treatments for peri-implantitis are available, but their cost-effective
119 d with subgingival plaque from patients with peri-implantitis are evaluated in terms of: 1) plaque an
120 logic factors for peri-implant mucositis and peri-implantitis are presented, including: foreign body
121   The main bacterial species associated with peri-implantitis are recognized as periodontal pathogens
122 e designs affecting the early progression of peri-implantitis are scarce.
123 ribution of the cell population was found in peri-implantitis around CI compared with TI.
124                                              Peri-implantitis around CI in comparison with TI seems t
125 diation for regenerative surgical therapy of peri-implantitis-associated osseous defects.
126                   This constituted a drop in peri-implantitis at both patient and implant level of ne
127 s demonstrated to influence the incidence of peri-implantitis at implant but not patient level.
128 ht of evidence for microorganisms related to peri-implantitis based on results of association studies
129 he decontamination of titanium implants with peri-implantitis, based on their antimicrobial effect.
130                                              Peri-implantitis begins to appear more frequently after
131 nd in increased count/abundance/frequency in peri-implantitis belonged to Bacteria domain and viruses
132                             Thirty-six human peri-implantitis biopsies were analyzed using light micr
133 and management of peri-implant mucositis and peri-implantitis by periodontists in the United States.
134  >=1 implant who were surgically treated for peri-implantitis by resective therapy.
135 overing (week 28); induction of experimental peri-implantitis by the use of three ligatures (weeks 31
136 nsufficient for a clear conclusion regarding peri-implantitis cases.
137 samples were collected from 85 patients with peri-implantitis (cases) and from 69 patients with only
138 nical outcomes of a concept for non-surgical peri-implantitis combining stepwise mechanical debrideme
139 nical outcomes of a concept for non-surgical peri-implantitis combining stepwise mechanical debrideme
140  microbial profiles or entire microbiomes of peri-implantitis compared with healthy implants or perio
141 ed in submucosal plaque around implants with peri-implantitis compared with healthy implants, indicat
142 ere significantly increased in patients with peri-implantitis compared with patients with healthy per
143 ) for mucositis and OR 15.26 (P = 0.001) for peri-implantitis, compared with subjects without MetS, w
144  frequent finding and that the prevalence of peri-implantitis correlates with loading time.
145 ium brush in the reconstructive treatment of peri-implantitis could enhance long-term outcomes.
146 t in comparison to conventional treatment of peri-implantitis could not be identified.
147                                 For example, peri-implantitis defects >=50% and 25% to 50% MBL were 1
148 gical approaches have been proposed to treat peri-implantitis defects with limited effectiveness and
149 sue breakdown and at regeneration of bone in peri-implantitis defects.
150              A trend of higher prevalence of peri-implantitis defined by detectable RBL beyond the ph
151                 Forty hopeless implants with peri-implantitis designated for removal were included in
152 p and miRNA-150-5p could be related with the peri-implantitis development.
153 A-21-3p and miRNA-150-5p was associated with peri-implantitis diagnosis (OR:0.23, CI 0.08-0.66, P = 0
154                 Although not associated with peri-implantitis diagnosis risk, keratinized mucosa (KM)
155                    The mean follow-up before peri-implantitis diagnosis was 99.47 +/- 47.93 months.
156  shown to significantly increase the risk of peri-implantitis diagnosis.
157                                              Peri-implantitis did not differ significantly from mucos
158 cause peri-implant mucositis may progress to peri-implantitis, effective treatment resulting in resol
159 ears, seven males/eight females) with severe peri-implantitis (eight CI, seven TI).
160                             The incidence of peri-implantitis exhibited a peak rate after the seventh
161                           Due to the risk of peri-implantitis, following dental implant placement, th
162 ory of periodontal disease were obtained for peri-implantitis for both implant and patient levels.
163 d Td levels were significantly higher in the peri-implantitis group (P <0.05).
164  concentration of titanium was higher in the peri-implantitis group compared with the group without p
165           Patients with type 2 diabetes with peri-implantitis (group A), non-diabetic individuals wit
166  (group B), and individuals with and without peri-implantitis (group C) were included.
167 ed into healthy, peri-implant mucositis, and peri-implantitis groups.
168                                Implants with peri-implantitis harbored significantly higher mean leve
169                         At the present time, peri-implantitis has become a global burden that occurs
170 uring the past decade, and the prevalence of peri-implantitis has increased.
171  diseases, namely peri-implant mucositis and peri-implantitis, have been extensively studied.
172 c oral infections, such as periodontitis and peri-implantitis, have complex etiology and pathogenesis
173                      Implants diagnosed with peri-implantitis having 1- (T1) and 2-year (T2) follow-u
174 6-microm) laser in the surgical treatment of peri-implantitis; however, its use may be promising.
175  is to evaluate the prevalence of mucositis, peri-implantitis, implant success, and survival in parti
176  and exosomes was significantly increased in peri-implantitis implants compared to healthy implants (
177 cts with healthy, peri-implant mucositis and peri-implantitis implants.
178      The material included 382 implants with peri-implantitis in 150 patients.
179 P patients, mucositis was present in 56% and peri-implantitis in 26% of the implants.
180 significantly downregulated in patients with peri-implantitis in comparison with peri-implant mucosit
181 emical parameters in a model of experimental peri-implantitis in dogs, followed by open flap debridem
182 /=2 PIMT/year seems to be crucial to prevent peri-implantitis in healthy patients.
183 ntal implants, which suggests corrosion, and peri-implantitis in humans.
184 ent study aims to evaluate the prevalence of peri-implantitis in implants inserted in augmented maxil
185                                 Frequency of peri-implantitis in the survey was 17.8% at the particip
186 the prevalence of peri-implant mucositis and peri-implantitis in their practices is up to 25% but is
187 ositive anaerobic rod has been identified in peri-implantitis, in endodontic infections, and in patie
188                            The prevalence of peri-implantitis increased from 3.2% to 9.7% between 5 a
189                                              Peri-implantitis is a challenging condition to manage an
190                                              Peri-implantitis is a complex polymicrobial biofilm-indu
191                                              Peri-implantitis is a frequent finding but estimates of
192                                              Peri-implantitis is an inflammatory condition that can l
193                                              Peri-implantitis is associated with younger ages and dia
194                                Prevalence of peri-implantitis is directly proportional to the time of
195 uvant antibiotic therapy in the treatment of peri-implantitis is not well understood.
196  knowledge, a standard protocol for treating peri-implantitis is not yet established.
197                                              Peri-implantitis is the leading cause for IR.
198 duction of these materials and their role in peri-implantitis is unknown.
199                                              Peri-implantitis is widely recognized as a major cause o
200       Differences in cellular composition of peri-implantitis lesions might also depend on the patien
201 methyladenosine [m6Am]) in periodontitis and peri-implantitis lesions, playing vital roles in the inn
202 ve abundance of Eubacterium was increased at peri-implantitis locations, and co-occurrence analysis r
203     Increasing preclinical data suggest that peri-implantitis microbiota not only triggers an inflamm
204 ere not detected continuously as part of the peri-implantitis microbiota.
205 ncluding surgical trauma, occlusal overload, peri-implantitis, microgap, biologic width, and implant
206 (n = 10), peri-implant mucositis (n = 8) and peri-implantitis (n = 6) sites using pyrosequencing of t
207 ial role of titanium dissolution products in peri-implantitis necessitate the consideration of materi
208 ntitis group compared with the group without peri-implantitis; no traces of titanium were observed in
209 of the implants and 48% of the patients, and peri-implantitis occurred in 16% of the implants and 26%
210  the implants and 52.2% of the subjects, and peri-implantitis occurred in 8.7% of the implants and 15
211                                           If peri-implantitis occurred, 11 treatment strategies (non-
212                           In the presence of peri-implantitis, only bleeding on probing at the adjace
213 s substantially associated with frequency of peri-implantitis (OR = 0.13, P = 0.01).
214  with peri-implant mucositis (OR = 4.33) and peri-implantitis (OR = 9.00).
215 nificantly correlated with the occurrence of peri-implantitis (P <0.001).
216 ignificant differences between mucositis and peri-implantitis patients (p = 0.001).
217                                              Peri-implantitis patients with implant pocket depths (IP
218 7.92% in the total sample size and 54.38% in peri-implantitis patients.
219 randomized controlled trial was conducted in peri-implantitis patients.
220 ic review assesses microbiologic profiles of peri-implantitis, periodontitis, and healthy implants ba
221  the implant group was 26.1%, largely due to peri-implantitis (PI), compared to 9.1% in the PR group
222 pact of these surfaces on the development of peri-implantitis (PI).
223  into those diagnosed with (test) or without peri-implantitis (PIm) (control).
224 ition (HI), peri-implant mucositis (PIM) and peri-implantitis (PIMP) by assessing respective diagnost
225 clinical questions: 1) whether patients with peri-implantitis (PP) present higher prevalence of any s
226 dies have implicated prostaglandin E2 in the peri-implantitis process, opening the possibility to man
227 -implant status after surgical treatment for peri-implantitis provides a framework for diagnosing the
228                            The prevalence of peri-implantitis ranges between 15% and 20% after 10 y,
229 between 5 and 10 years of follow-up, and the peri-implantitis rate among implants was 12.9% after 10
230 ntly higher prevalence of moderate to severe peri-implantitis (RBL >=2 mm).
231 the effectiveness of a titanium brush in the peri-implantitis reconstructive treatment.
232 udy indicated using laser irradiation during peri-implantitis regenerative therapy may aid in better
233         HA reduced the relative abundance of peri-implantitis-related microorganisms, especially the
234                                              Peri-implantitis represents a disruption of the biocompa
235                                              Peri-implantitis represents a heterogeneous mixed infect
236          The use of HA in advanced stages of peri-implantitis resulted in a decrease in microbial alp
237 etiologic factors associated with retrograde peri-implantitis (RPI) and potential treatment options h
238                                   Retrograde peri-implantitis (RPI) is a rapidly progressing periapic
239                          Although retrograde peri-implantitis (RPI) is not a common sequela of dental
240 significantly higher values of sclerostin in peri-implantitis samples.
241                                Patients with peri-implantitis showed statistically significantly bett
242                                              Peri-implantitis sites were also colonized by uncultivab
243 irochete levels were significantly higher at peri-implantitis sites when compared with levels at peri
244 was correlated with Prevotella intermedia in peri-implantitis sites, which suggests the association o
245 ermedius/nigrescens were often identified at peri-implantitis sites.
246 oorganisms were not found very frequently in peri-implantitis sites.
247 om plaque samples obtained from experimental peri-implantitis sites.
248 ficantly with probing depth and bone loss at peri-implantitis sites.
249             Postoperative complications were peri-implantitis (six cases) and osseointegration losses
250  after implant placement (T0) and the day of peri-implantitis surgical treatment (T1).
251 tients with and without type 2 diabetes with peri-implantitis than systemically healthy individuals w
252 ial was performed in patients diagnosed with peri-implantitis that exhibited contained defects.
253                                Patients with peri-implantitis that were treated with an intensive tre
254 ch procedure RESULTS: Following experimental peri-implantitis, the dynamics of renal parameters and b
255 eatment methods were influential in treating peri-implantitis, the laser group (MD+Er,Cr:YSGG) yielde
256             After regenerative treatment for peri-implantitis, the peri-implant condition was classif
257 in was proposed for use in periodontitis and peri-implantitis therapy due to its bone-supportive effe
258                     The effectiveness of the peri-implantitis therapy was impaired by severe periodon
259  months of follow-up in >/= 10 patients with peri-implantitis treated with lasers were included.
260 nin as a promising drug in periodontitis and peri-implantitis treatment.
261 t consideration in the clinical selection of peri-implantitis treatments and a necessary criterion fo
262                                              Peri-implantitis treatments are mainly based on protocol
263 icles evaluated the microbiologic profile of peri-implantitis versus healthy implants or periodontiti
264 lants, respectively, while the prevalence of peri-implantitis was 10.1% at the patient level and 5.4%
265                             The incidence of peri-implantitis was 8%, while the incidence of RPI was
266                                      Risk of peri-implantitis was assumed to be affected by SIT and t
267                                              Peri-implantitis was defined as presence of pocket depth
268                                              Peri-implantitis was defined as radiographic bone loss o
269                                              Peri-implantitis was defined as radiographic bone loss o
270                                              Peri-implantitis was defined based on the consensus repo
271 83 patients were enrolled: in MetS subjects, peri-implantitis was detected in 36.9% (n = 31) of impla
272 lant mucositis and preventing development of peri-implantitis was either provided or not.
273 her prevalence (48.8%) of moderate to severe peri-implantitis was identified in CVD compared with con
274  At the LM level, the inflammatory lesion of peri-implantitis was in most cases a mixture of subacute
275 ere connected to prostheses and experimental peri-implantitis was induced by ceasing scaling procedur
276 e full documentation in which no evidence of peri-implantitis was not indicated.
277 5% confidence interval [CI]: 1.003-4.63) for peri-implantitis was observed in implants supporting rem
278 t, the survival rate of implants treated for peri-implantitis was primarily influenced by the amount
279 Furthermore, the prevalence of mucositis and peri-implantitis was shown to be lower at both the impla
280                                              Peri-implantitis was the main reason for IR (64.5%).
281 icipants and 30.7% of implants, and those of peri-implantitis were 18.8% of participants and 9.6% of
282 The prevalence of peri-implant mucositis and peri-implantitis were 82.1% and 41.4% at the subject lev
283  animal studies applying lasers for treating peri-implantitis were also included.
284 dontitis, healthy implants, or implants with peri-implantitis were colonized by periodontal microorga
285                  Additionally, the risks for peri-implantitis were evaluated from the perspective of
286 tis comprising 164 screw-typed implants with peri-implantitis were included.
287 and a total of 164 screw-typed implants with peri-implantitis were included.
288           Putative pathogens associated with peri-implantitis were present at a moderate relative abu
289         Criteria for successful treatment of peri-implantitis were proposed.
290 ents who underwent non-surgical treatment of peri-implantitis were randomly divided into two groups.
291                             Individuals with peri-implantitis were twice as likely to report a proble
292       Overall, 11.9% of the participants had peri-implantitis, whereas 68.9% had peri-implant mucosit
293 curred in the early post-diagnosis period of peri-implantitis, which could be affected by the restora
294          Twenty-four patients diagnosed with peri-implantitis with a radiographic infrabony defect we
295 the first bone-to-implant contact, extensive peri-implantitis with advanced bone resorption, and exte
296 surgical outcomes of resective treatment for peri-implantitis with and without implant surface modifi
297 t 45 days on the microbiome of implants with peri-implantitis with at least 1 year of loading.
298          QoL was impaired by the presence of peri-implantitis with high level of concern and low leve
299 d GAgP are more susceptible to mucositis and peri-implantitis, with lower implant survival and succes
300 betes and peri-implantitis and patients with peri-implantitis without diabetes.

 
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