Safety of Oral Bisphosphonates: Controlled Studies on Alveolar Bone Purpose: Osteoporosis and osteopenia are characterized by reductions in bone mass and may lead toskeletal fragility and fracture. The latest generation of oral bisphosphonate drugs, including alen-dronate and risendronate, has been approved for the prevention and treatment of osteoporosis. Thesemedications are chemically absorbed into bone, decreasing osteoclast number and activity andthereby decreasing bone resorption. The purpose of this report is to present safety data from 2 con-trolled studies in patients receiving oral bisphosphonates. Materials and Methods: Study 1 tested theeffect of alendronate, an inhibitor of bone resorption, on alveolar bone. A total of 335 patients (162men and 173 women, aged 30 to 79 years) with moderate or severe periodontal disease were ran-domized to either placebo or 70 mg alendronate once weekly. Alveolar bone height and safety wereassessed over a 2-year period. Study 2 was a longitudinal single-blind controlled design comparingimplant success in 50 consecutive patients (210 implants), 25 patients who received bisphosphonatetherapy and 25 age-matched control subjects. Implant success and safety, including incidence ofosteonecrosis of the jaws (ONJ), was blindly assessed for at least 3 years. Results: In study 1, nocases of ONJ were observed in either treatment group. Furthermore, a trend toward lower incidencesof infection and tooth loss was observed in the alendronate group. In study 2, no cases of ONJ wereobserved in either group, and implant success was greater than 99% in both groups. Conclusion: Onthe basis of 2 controlled clinical studies, oral bisphosphonate usage was not associated with occur-rence of ONJ. (Controlled Clinical Study) INT J ORAL MAXILLOFAC IMPLANTS 2006;21:349–353
Key words: alveolar bone, bisphosphonates, clinical trials, implants, periodontal disease, treatment
Osteoporosis and osteopenia are characterized by menopause, thin or small body frame, race, and
reductions in bone mass and may lead to skele-
heredity. Lack of calcium intake, lack of exercise,
tal fragility and fracture. In 1994 the World Health
smoking, and alcohol are modifiable risk factors. Low
Organization defined osteoporosis as a bone mineral
bone mass, certain medications, and systemic dis-
density (BMD) level more than 2.5 standard devia-
eases such as hyperparathyroidism are modifiable to
tions below the mean of normal young women.1
some extent. Many of the risk factors for osteoporo-
Risk factors for osteoporosis can be categorized as
sis are similar to risk factors for dental implant
nonmodifiable or modifiable.1,2 The nonmodifiable
risk factors for osteoporosis include sex, age, early
Bone loss in women occurs most rapidly in the
years immediately following menopause, when nat-ural levels of estrogen are greatly reduced. In mostwomen, bone mass reaches its peak in the thirddecade of life (around 25 to 35 years of age) and
1Morton Amsterdam Dean and Professor, University of Pennsylva-
declines thereafter. This decline in bone mass accel-
nia School of Dental Medicine, Philadelphia, Pennsylvania.
erates with the onset of menopause.3,4 While esti-mates of the rate of postmenopausal bone loss may
Correspondence to: Dr Marjorie K. Jeffcoat, University of Penn-
differ by population and measurement technology, a
sylvania School of Dental Medicine, 240 S. 40th Street, Philadel-phia, PA 19104. Fax: +215 573 4075. E-mail:
rate of about 0.5% to 1.0% per year has been
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Osteoporosis is not a substantial health risk, but
coded for blind assessment of alveolar evidence, and
treatment of osteoporosis is important to the health
presence of ONJ and radiolucency. Thus, assessment
of patients. Nearly 50% of women develop osteo-
of the radiographs was completed by a single inves-
porosis. Furthermore, almost 24% of women who suf-
tigator with no knowledge of the treatment group
fer a hip fracture die within a year due to sequellae of
or the patient’s clinical adherence to the study regi-
the fracture. Therefore, prevention and treatment of
men. Other tooth-related safety data, such as caries
osteoporosis is an important part of the chemothera-
and gingival index (GI) data, have been reported
peutic regimen for patients who may be candidates
elsewhere.16 No adverse pattern of events was
for dental implants. Recent case repor ts have
included observations of osteonecrosis of the jaws
The primary efficacy endpoint was the change in
(ONJ) in patients receiving bisphosphonates.5–12
ABH. ABH is defined as the distance between the
However, in the vast majority of these cases, bisphos-
cementoenamel junction (CEJ) and the alveolar bone
phonate drugs were administered intravenously
crest. In normal conditions, the level of the crest is 1
rather than taken orally for the prevention and treat-
Statistical Evaluation. Safety data was tabulated
The purpose of this report is to present safety data
but not amenable to statistical analysis due to the
from 2 controlled studies of oral bisphosphonates.
low level of adverse events in both the placebo andalendronate groups.
Changes in ABH from baseline were analyzed by
the analysis-of-variance method (ANOVA), includingtreatment group and study center as factors. Treat-
ment-by-center interaction was not found to be sig-
The first study was a double-blind placebo-con-
nificant at the .05 level. Analyses were performed on
trolled study of the safety of oral alendronate taken
per-patient summaries of the measurements at qual-
on a once-weekly basis. The study was designed to
ified tooth sites for each individual patient.
explore the effects of alendronate, a potent inhibitorof bone resorption, on alveolar bone loss in patients
with moderate or severe periodontal disease.13 The
Baseline Characteristics. A total of 162 men and 173
rationale for the study was based on the fact that
women were enrolled in the study. The patients
periodontal bone loss is mediated by osteoclasts,
ranged in age from 30 to 79 years (mean, 50 years).
whose function is selectively inhibited by alen-
Approximately 75% of the patients enrolled were
dronate.6 Alendronate had previously been shown to
Caucasian, while 17% were African Americans. Sixty-
decrease periodontal bone loss in 2 animal models
two percent were smokers, and 71% of the patients
of periodontal disease14,15 and to decrease loss of
had severe periodontal disease. Only 3% were dia-
alveolar bone height and density in a small number
betic. There were no differences between groups in
of subjects with moderate periodontal disease.9 The
Efficacy. Figure 1 shows the ABH at baseline and
A total of 335 patients (age range, 30 to 79 years)
after 2 years in subjec ts with low and normal
with moderate or severe periodontal disease were
mandibular BMD. A significant gain in ABH was seen
enrolled in the study. Moderate to severe periodontal
in the alendronate-treated group (periodontal bone
disease was defined by the presence of pocketing,
loss 4.16 ± .11 mm baseline, 3.75 ± .18 mm 2 years)
loss in clinical attachment, and loss of at least 3 mm
relative to the placebo group (periodontal bone loss
of alveolar bone height (ABH). A diagnosis of osteo-
4.22 ± .13 mm baseline, 4.61 ± .23 mm 2 years) (P <
porosis was not an inclusion criterion for the study.
.001) in patients with low mandibular BMD at base-
Patients were randomized at 12 US sites to either 70
line. This significant difference was not observed in
mg alendronate or a placebo once weekly; they
alendronate-treated patients with normal BMD at
received nonsurgical periodontal treatment at the
baseline (4.33 ± 0.13 mm baseline, 4.49 ± 0.21 mm 2
time of randomization. Patients were examined at 2
years) compared with placebo-treated subjects (4.32
clinic visits (screening and baseline) prior to random-
± 0.11 mm baseline, 4.31 ± 0.18 mm 2 years).
ization and once every 3 months thereafter for 2
Safety. Table 1 shows the alveolar bone and perio-
years. Maintenance treatment was performed every
dontal safety profile. No cases of ONJ were observed
over the 2-year study period. In fact, fewer teeth were
The primary safety endpoint, or measure of safety,
lost in the bisphosphonate group, in spite of the
was ONJ. Infection and progressive alveolar bone
existence of periodontal disease at baseline, than in
loss were also considered. All radiographs were
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*Number of teeth lost shown rather than number of patients who lost
Effect of alendronate on alveolar bone. Bone loss from
the CEJ (mean ± SD) is shown for patients with low BMD at base-line versus those with normal BMD at baseline. Note a significantdecrease in bone loss16 in the alendronate-treated group in sub-jects with low BMD at baseline.
Results Analysis revealed that 100.0% of the implants placed
The second study was a parallel-arm controlled study
in patients receiving bisphosphonates were success-
of dental implant patients receiving oral bisphospho-
ful, compared with 99.2% in the group not receiving
nates versus control dental implant patients.
bisphosphonates (Fig 2). There was no significant dif-ference between the 2 study groups (P > .95).
Materials and MethodsDesign. This single-blind controlled study involved theconsecutive analysis of 3-year results from 25 patients
(102 implants) receiving oral bisphosphonates (alen-dronate or risendronate) versus 25 age-matched
A number of cases of ONJ following treatment with
patients (108 implants) who did not receive bisphos-
high-dose bisphosphonates, especially in cancer
phonates. All patients were postmenopausal women
patients treated parenterally and in the presence of
with BMD scores indicative of osteoporosis. Only 1
additional risk factors such as chemotherapy, gluco-
patient per study arm smoked. Patients in the bisphos-
cor ticoids, and poor oral hygiene, have been
phonate arm had taken the drug for 1 to 4 years (mean
reported to regulatory agencies.5–12 Patients receiv-
3 ± 0.1 years) prior to inclusion in the study.
ing intravenous bisphosphonate therapy were not
Following implant placement, patients were fol-
studied as part of the present study. This smaller
lowed for at least 3 years with oral examinations,
population with especially complex medical prob-
radiographs, and routine maintenance. Two-stage
lems is deserving of controlled studies.
osseointegrated implants were used in all patients.
The present study is, thus far, the largest random-
Fixed screw-retained prostheses were placed and
ized, placebo-controlled study of an antiresorptive
removed to assess implant mobility, which was
agent in patients with oral disease that was designed
to assess oral side effects and outcomes in a blinded
Outcomes. Coded digital radiographs were used
controlled manner. After 2 years of treatment, a sig-
to provide yearly measurements of bone loss and
nificant positive effect of alendronate was observed
were examined for evidence of ONJ. Calibrated clini-
relative to placebo in the subgroup of patients with
cians also measured mobility and assessed clinical
evidence of pain, infection, and ONJ.
Other investigators have reported positive results
Statistical Analysis. A Kaplan-Meier analysis was
with alendronate therapy, primarily on ABH and alveolar
used to compare the success rate of implants in
bone density, with daily doses equivalent to the weekly
patients receiving oral bisphosphonates to implants
dose used in the current study.16–22 However, the dura-
in patients not receiving oral bisphosphonates. Suc-
tion of follow-up in these studies was only 6 months.
cess was defined as less than 2 mm of alveolar bone
Study 1 also provided additional data on the
loss over the 3-year study period, lack of mobility,
safety of once-weekly alendronate. As previously
lack of infection, and absence of pain and ONJ.
observed in a study of postmenopausal women,20,23
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be missing a greater number of teeth than post-menopausal women with normal BMD.23 Therefore,
given the large number of women routinely takingoral bisphosphonates and the relatively few cases ofosteonecrosis seen in the present sample, it appearsthat the small risk of developing osteonecrosis
should be considered with due regard for the poten-
tial benefits (retardation of alveolar bone loss).
The decision to proceed with any medical or dental
Implant success in bisphosphonate-treated and control
procedure, be it prescription of oral bisphosphonates
patients. One hundred percent of implants in patients receivingoral bisphosphonate met the success criteria, and 99.2% of
or placement of a dental implant, involves balancing
implants in patients not receiving the drug were successful.
the risks against the benefits and making choices. Osteoporosis is a serious bone disease requiringtreatment in the absence of major risks. In the 2 con-trolled studies presented, oral bisphosphonates werenot found to pose a risk to alveolar bone comparedto placebo.
70 mg oral alendronate once weekly was generallysafe and well tolerated. This favorable safety profile
included maxillar y gingival index and dental adverse experiences. This study supports prior
The authors thank Proctor and Gamble Pharmaceutical for par-
research17–19,21,22 and shows both reduced rates of
tially funding study 2 by providing a Grant in Aid for data analysis. The authors also thank Merck Research for access to a multicen-
bone loss and reduced bone loss with absence of ONJ
in a multicenter study population. However, it isacknowledged that, given the relatively long half-lifeof bisphosphonates, the long-term effects of alen-
dronate therapy cannot be determined from the 2- to3-year follow-up presented here.
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HOMENAJE A SIGMUND FREUD EN EL 150 ANIVERSARIO DE SU NACIMIENTO EL HOMBRE DE LOS LOBOS Una aproximación Gestáltica a un paciente de Sigmund Freud I. INTRODUCCIÓN Estoy teniendo la osadía de escribir este ensayo a 150 años del nacimiento del padre del psicoanálisis, y por consiguiente el abuelo de todas las psicoterapias que se han construido a la sombra protectora de s
Science, Art and Drug Discovery, A Personal Perspective Simon F. Campbell, PhD FRS Formerly Senior Vice President, WW Discovery, Pfizer Central Research The pharmaceutical industry is under intense pressure to increase productivity, and drug discovery is undergoing a paradigm shift whereby the explosion in genome sciences and new technologies is being harnessed to produce innovative th