Jungtinės Valstijos - anglų - NLM (National Library of Medicine)

aurobindo pharma limited - risedronate sodium (unii: ofg5exg60l) (risedronic acid - unii:km2z91756z) - risedronate sodium tablets are indicated for the treatment and prevention of osteoporosis in postmenopausal women. in postmenopausal women with osteoporosis, risedronate sodium tablets reduce the incidence of vertebral fractures and a composite endpoint of nonvertebral osteoporosis-related fractures [see clinical studies (14.1, 14.2)] . risedronate sodium tablets are indicated for treatment to increase bone mass in men with osteoporosis. risedronate sodium tablets are indicated for the treatment and prevention of glucocorticoid-induced osteoporosis in men and women who are either initiating or continuing systemic glucocorticoid treatment (daily dosage of greater than or equal to 7.5 mg of prednisone or equivalent) for chronic diseases. patients treated with glucocorticoids should receive adequate amounts of calcium and vitamin d. risedronate sodium tablets are indicated for treatment of paget’s disease of bone in men and women. the optimal duration of use has not been determined. the safety and effectiveness of risedronate sodium tablets for the treatment of osteoporosis are based on clinical data of three years duration. all patients on bisphosphonate therapy should have the need for continued therapy re-evaluated on a periodic basis. patients at low-risk for fracture should be considered for drug discontinuation after 3 to 5 years of use. patients who discontinue therapy should have their risk for fracture re-evaluated periodically. risedronate sodium tablets are contraindicated in patients with the following conditions: - abnormalities of the esophagus which delay esophageal emptying such as stricture or achalasia [see warnings and precautions (5.1)] - inability to stand or sit upright for at least 30 minutes [see dosage and administration (2), warnings and precautions (5.1)] - hypocalcemia [see warnings and precautions (5.2)] - known hypersensitivity to risedronate sodium tablets or any of its excipients. angioedema, generalized rash, bullous skin reactions, stevens-johnson syndrome and toxic epidermal necrolysis have been reported [see adverse reactions (6.2)] risk summary available data on the use of risedronate in pregnant women are insufficient to inform a drug-associated risk of adverse maternal or fetal outcomes. discontinue risedronate when pregnancy is recognized. in animal reproduction studies, daily oral administration of risedronate to pregnant rats during organogenesis decreased neonatal survival and body weight at doses approximately 5 and 26 times, respectively, the highest recommended human daily dose of 30 mg (based on body surface area, mg/m2 ). a low incidence of cleft palate was observed in fetuses of dams treated at doses approximately equal to the 30 mg human daily dose. delayed skeletal ossification was observed in fetuses of dams treated at approximately 2.5 to 5 times the 30 mg human daily dose. periparturient mortality due to maternal hypocalcemia occurred in dams and neonates upon daily oral administration of risedronate to pregnant rats during mating and/or gestation starting at doses equivalent to the 30 mg daily human dose. bisphosphonates are incorporated into the bone matrix, from which they are gradually released over a period of years. the amount of bisphosphonate incorporated into adult bone and available for release into the systemic circulation is directly related to the dose and duration of bisphosphonate use. consequently, based on the mechanism of action of bisphosphonates, there is a potential risk of fetal harm, predominantly skeletal, if a woman becomes pregnant after completing a course of bisphosphonate therapy. the impact of variables such as time between cessation of bisphosphonate therapy to conception, the particular bisphosphonate used, and the route of administration (intravenous versus oral) on this risk has not been studied. the estimated background risk of major birth defects and miscarriage for the indicated populations is unknown. all pregnancies have a background risk of birth defects, loss, or other adverse outcomes. in the u.s. general population, the estimated background risks of major birth defects and miscarriage in clinically recognized pregnancies is 2 to 4% and 15 to 20%, respectively. data animal data in animal studies, pregnant rats received risedronate sodium during organogenesis at doses equivalent to 1 to 26 times the 30 mg human daily dose (based on body surface area, mg/m2 ). survival of neonates was decreased in dams treated during gestation with oral doses approximately 5 times the human dose, and body weight was decreased in neonates of dams treated with approximately 26 times the human dose. a low incidence of cleft palate was observed in fetuses of dams treated with oral doses approximately equal to the human dose. the number of fetuses exhibiting incomplete ossification of sternebrae or skull of dams treated with approximately 2.5 times the human dose was significantly increased compared to controls. both incomplete ossification and unossified sternebrae were increased in fetuses of dams treated with oral doses approximately 5 times the human dose. no significant ossification effects were seen in fetuses of rabbits treated with oral doses approximately 7 times the human dose (the highest dose tested). however, 1 of 14 litters were aborted and 1 of 14 litters were delivered prematurely. periparturient mortality due to maternal hypocalcemia occurred in dams and neonates when pregnant rats were treated daily during mating and/or gestation with oral doses equivalent to the human dose or higher. risk summary there are no data on the presence of risedronate in human milk, the effects on the breastfed infant, or the effects on milk production. a small degree of lacteal transfer occurred in nursing rats. the concentration of the drug in animal milk does not necessarily predict the concentration of drug in human milk. however, when a drug is present in animal milk, it is likely that the drug will be present in human milk. the developmental and health benefits of breast-feeding should be considered along with the mother’s clinical need for risedronate and any potential adverse effects on the breast-fed child from risedronate or from the underlying maternal condition. data animal data risedronate was detected in neonates of lactating rats given a single oral dose of risedronate at 24-hours post-dosing, indicating a small degree of lacteal transfer. risedronate is not indicated for use in pediatric patients. the safety and effectiveness of risedronate was assessed in a one-year, randomized, double-blind, placebo-controlled study of 143 pediatric patients (94 received risedronate) with osteogenesis imperfecta (oi). the enrolled population was predominantly patients with mild osteogenesis imperfecta (85% type-i), aged 4 to less than 16 years, 50% male and 82% caucasian, with a mean lumbar spine bmd z-score of -2.08 (2.08 standard deviations below the mean for age-matched controls).  patients received either a 2.5 mg (less than or equal to 30 kg body weight) or 5 mg (greater than 30 kg body weight) daily oral dose. after one year, an increase in lumbar spine bmd in the risedronate group compared to the placebo group was observed. however, treatment with risedronate did not result in a reduction in the risk of fracture in pediatric patients with osteogenesis imperfecta. in risedronate-treated subjects, no mineralization defects were noted in paired bone biopsy specimens obtained at baseline and month 12. the overall safety profile of risedronate in oi patients treated for up to 12 months was generally similar to that of adults with osteoporosis. however, there was an increased incidence of vomiting compared to placebo. in this study, vomiting was observed in 15% of children treated with risedronate and 6% of patients treated with placebo. other adverse events reported in greater than or equal to 10% of patients treated with risedronate and with a higher frequency than placebo were: pain in the extremity (21% with risedronate versus 16% with placebo), headache (20% versus 8%), back pain (17% versus 10%), pain (15% versus 10%), upper abdominal pain (11% versus 8%), and bone pain (10% versus 4%). of the patients receiving risedronate in postmenopausal osteoporosis studies [see clinical studies (14)] , 47% were between 65 and 75 years of age, and 17% were over 75. the corresponding proportions were 26% and 11% in glucocorticoid-induced osteoporosis trials, and 40% and 26% in paget’s disease trials. no overall differences in efficacy between geriatric and younger patients were observed in these studies. in the male osteoporosis trial, 28% of patients receiving risedronate were between 65 and 75 years of age and 9% were over 75. the lumbar spine bmd response for risedronate compared to placebo was 5.6% for subjects less than 65 years and 2.9% for subjects greater than or equal to 65 years. no overall differences in safety between geriatric and younger patients were observed in the risedronate trials, but greater sensitivity of some older individuals cannot be ruled out. risedronate is not recommended for use in patients with severe renal impairment (creatinine clearance less than 30 ml/min) because of lack of clinical experience. no dosage adjustment is necessary in patients with a creatinine clearance greater than or equal to 30 ml/min. no studies have been performed to assess risedronate’s safety or efficacy in patients with hepatic impairment. risedronate is not metabolized in human liver preparations. dosage adjustment is unlikely to be needed in patients with hepatic impairment.

Jungtinės Valstijos - anglų - NLM (National Library of Medicine)

sciegen pharmaceuticals, inc. - valsartan (unii: 80m03yxj7i) (valsartan - unii:80m03yxj7i) - valsartan tablets are indicated for the treatment of hypertension, to lower blood pressure in adults and pediatric patients six years of age and older. lowering blood pressure reduces the risk of fatal and nonfatal cardiovascular events, primarily strokes and myocardial infarctions. these benefits have been seen in controlled trials of antihypertensive drugs from a wide variety of pharmacologic classes, including the class to which valsartan principally belongs. there are no controlled trials in hypertensive patients demonstrating risk reduction with valsartan tablets. control of high blood pressure should be part of comprehensive cardiovascular risk management, including, as appropriate, lipid control, diabetes management, antithrombotic therapy, smoking cessation, exercise, and limited sodium intake. many patients will require more than one drug to achieve blood pressure goals. for specific advice on goals and management, see published guidelines, such as those of the national high blood pressure education

Jungtiniai Arabų Emyratai - anglų - MOHAP (Ministry of Health & Prevention) - وزارة الصحة ووقاية المجتمع.الإمارات

triangle medical trading l.l.c. united arab emirates - 30's (30's blisters x 1) - tablet - 10,000 i.u. /tablet - nutrition , blood-vitamins

Jungtiniai Arabų Emyratai - anglų - MOHAP (Ministry of Health & Prevention) - وزارة الصحة ووقاية المجتمع.الإمارات

triangle medical trading l.l.c. united arab emirates - 30's (30's blisters x 1) - tablet - 10,000 i.u. /tablet - nutrition , blood-vitamins

Jungtiniai Arabų Emyratai - anglų - MOHAP (Ministry of Health & Prevention) - وزارة الصحة ووقاية المجتمع.الإمارات

triangle medical trading l.l.c. united arab emirates - 30's (30's blisters x 1) - tablet - 10,000 i.u. /tablet - nutrition , blood-vitamins

Jungtiniai Arabų Emyratai - anglų - MOHAP (Ministry of Health & Prevention) - وزارة الصحة ووقاية المجتمع.الإمارات

triangle medical trading l.l.c. united arab emirates - 30's (30's blisters x 1) - tablet - 10,000 i.u. /tablet - nutrition , blood-vitamins

Jungtiniai Arabų Emyratai - anglų - MOHAP (Ministry of Health & Prevention) - وزارة الصحة ووقاية المجتمع.الإمارات

triangle medical trading l.l.c. united arab emirates - 30's (30's blisters x 1) - tablet - 10,000 i.u. /tablet - nutrition , blood-vitamins

Jungtiniai Arabų Emyratai - anglų - MOHAP (Ministry of Health & Prevention) - وزارة الصحة ووقاية المجتمع.الإمارات

triangle medical trading l.l.c. united arab emirates - 30's (30's blisters x 1) - tablet - 10,000 i.u. /tablet - nutrition , blood-vitamins

Jungtinės Valstijos - anglų - NLM (National Library of Medicine)

alembic pharmaceuticals inc. - modafinil (unii: r3uk8x3u3d) (modafinil - unii:r3uk8x3u3d) - modafinil 100 mg - modafinil tablets are indicated to improve wakefulness in adult patients with excessive sleepiness associated with narcolepsy, obstructive sleep apnea (osa), or shift work disorder (swd). limitations of use in osa, modafinil tablets are indicated to treat excessive sleepiness and not as treatment for the underlying obstruction. if continuous positive airway pressure (cpap) is the treatment of choice for a patient, a maximal effort to treat with cpap for an adequate period of time should be made prior to initiating and during treatment with modafinil tablets for excessive sleepiness. modafinil tablets are contraindicated in patients with known hypersensitivity to modafinil or armodafinil or its inactive ingredients [see warnings and precautions (5.1, 5.2, 5.3)] . pregnancy category c there are no adequate and well-controlled studies of modafinil in pregnant women. intrauterine growth restriction and spontaneous abortion have been reported in association with modafinil (a mixture of r-and s-modafinil) and armod

Jungtinės Valstijos - anglų - NLM (National Library of Medicine)

eisai inc. - lemborexant (unii: 0k5743g68x) (lemborexant - unii:0k5743g68x) - dayvigo is indicated for the treatment of adult patients with insomnia, characterized by difficulties with sleep onset and/or sleep maintenance [see clinical studies ( 14.1 )] . dayvigo is contraindicated in patients with narcolepsy. pregnancy exposure registry there is a pregnancy exposure registry that monitors pregnancy outcomes in women who are exposed to dayvigo during pregnancy. healthcare providers are encouraged to register patients in the dayvigo pregnancy registry, a part of the national pregnancy registry for psychiatric medications, at1-866-961-2388 or online at https://womensmentalhealth.org/research/pregnancyregistry. risk summary there are no available data on dayvigo use in pregnant women to evaluate for drug-associated risks of major birth defects, miscarriage or adverse maternal or fetal outcomes. in animal reproduction studies, oral administration of lemborexant to pregnant rats and rabbits during the period of organogenesis caused toxicities only at high multiples of the human exposure at the maximum recommended human dose (mrhd) based on auc. the no observed adverse effect levels (noael) are approximately >100 and 23 times the mrhd based on auc in rats and rabbits, respectively. similarly, oral administration of lemborexant to pregnant and lactating rats caused toxicities only at high multiples of the human exposure at the mrhd based on auc. the noael is 93 times the mrhd based on auc ( see data ) . the estimated background risk of major birth defects and miscarriage for the indicated population is unknown. all pregnancies have a background risk of birth defect, loss, or other adverse outcomes. in the u.s. general population, the estimated background risks of major birth defects and miscarriage in clinically recognized pregnancies are 2% to 4% and 15% to 20%, respectively. data animal data lemborexant was administered orally to pregnant rats during the period of organogenesis in 2 studies at doses of 60, 200, and 600 mg/kg/day or 20, 60, and 200 mg/kg/day, which are approximately 6 to >300 times the mrhd based on auc. lemborexant caused maternal toxicity, manifested by decreased body weight and food consumption, decreased mean fetal body weight, an increased number of dead fetuses, and skeletal, external and visceral malformations (omphalocele, cleft palate, and membranous ventricular septal defect) at >300 times the mrhd based on auc. the noael of 200 mg/kg/day is approximately 143 times the mrhd based on auc. lemborexant was administered orally to pregnant rabbits during the period of organogenesis at doses of 10, 30, and 100 mg/kg/day, which are approximately 7 to 139 times the mrhd based on auc. lemborexant caused maternal toxicity that consisted of decreased body weight and food consumption and a higher incidence of skeletal variations (presence of cervical ribs and supernumerary lung lobes) at approximately 139 times the mrhd based on auc. the noael of 30 mg/kg/day is approximately 23 times the mrhd based on auc. lemborexant was administered orally to pregnant rats during pregnancy and lactation at doses of 30, 100, and 300 mg/kg/day, which are approximately 15 to 206 times the mrhd based on auc. lemborexant caused maternal toxicity that consisted of decreased body weight and food consumption and toxicity to offspring consisting of decreased pup body weights, decreased femur length, and decreased acoustic startle responses at 206 times the mrhd based on auc. the noael of 100 mg/kg/day is approximately 93 times the mrhd based on auc. risk summary available data from a lactation study in 8 women indicates that lemborexant is transferred into the breastmilk of nursing mothers, and the results have established a mean daily infant dose of 0.0029 mg/kg/day and a relative infant dose of less than 2% of the maternal dose. these data support that transfer of lemborexant into breastmilk is low (see data). there are no data on the effects of lemborexant on the breastfed infant, or the effects on milk production. infants exposed to dayvigo through breastmilk should be monitored for excessive sedation. the developmental and health benefits of breastfeeding should be considered along with the mother’s clinical need for dayvigo and any potential adverse effects on the breastfed infant from dayvigo or from the underlying maternal condition. data a single dose milk-only lactation study was conducted in 8 healthy adult lactating women. the mean amount of lemborexant recovered in human milk was 0.0174 mg following a 10 mg maternal dose. the mean calculated daily infant oral dosage was 0.0029 mg/kg/day based on nominal infant body weight of 6 kg. approximately 70% of the total amount of lemborexant excreted in milk was excreted by 24 hours after a single maternal dose administration. there are no data on the effects of lemborexant on the breastfed infant, the effects on milk production, or infant exposure after repeated maternal dosing of lemborexant. the safety and effectiveness of dayvigo have not been established in pediatric patients. of the total number of patients treated with dayvigo (n=1418) in controlled phase 3 studies, 491 patients were 65 years and over, and 87 patients were 75 years and over. overall, efficacy results for patients <65 years of age were similar compared to patients ≥65 years. in a pooled analysis of study 1 (the first 30 days) and study 2, the incidence of somnolence in patients ≥65 years with dayvigo 10 mg was higher (9.8%) compared to 7.7% in patients <65 years. the incidence of somnolence with dayvigo 5 mg was similar in patients ≥65 years (4.9%) and <65 years (5.1%). the incidence of somnolence in patients treated with placebo was 2% or less regardless of age [see clinical studies ( 14.2 )].  because dayvigo can increase somnolence and drowsiness, patients, particularly the elderly, are at a higher risk of falls [see warning s and precautions ( 5.1 )] . exercise caution when using doses higher than 5 mg in patients ≥65 years old.  no dose adjustment is required in patients with mild, moderate, or severe renal impairment. dayvigo exposure (auc) was increased in patients with severe renal impairment. patients with severe renal impairment may experience an increased risk of somnolence [see clinical pharmacology ( 12.3 )]. dayvigo has not been studied in patients with severe hepatic impairment. use in this population is not recommended [see dosage and administration ( 2.3 ), clinical pharmacology ( 12.3 )].   dayvigo exposure (auc and cmax ) and terminal half-life were increased in patients with moderate hepatic impairment (child-pugh class b). dosage adjustment is recommended in patients with moderate hepatic impairment (child-pugh class b) [see dosage and administration ( 2.3 ), clinical pharmacology ( 12.3 )].   dayvigo exposure (auc) was increased in patients with mild hepatic impairment (child-pugh class a), but the terminal half-life was not changed. patients with mild hepatic impairment may experience an increased risk of somnolence [see clinical pharmacology ( 12.3 )]. obstructive sleep apnea (osa) the respiratory depressant effect of dayvigo was evaluated after 8 consecutive nights of treatment with dayvigo 10 mg in a randomized, placebo-controlled, two-period crossover study in 37 patients with mild osa (apnea-hypopnea index < 15 events per hour of sleep). following once daily dosing of 10 mg, the mean treatment difference (dayvigo – placebo) on day 8 for the apnea-hypopnea index was -0.06 (95% ci: -1.95 to 1.83). dayvigo was also evaluated after 8 consecutive nights of treatment with dayvigo 10 mg in a randomized, placebo-controlled, two-period crossover study in 33 patients with moderate to severe osa (apnea-hypopnea index ≥ 15 events per hour of sleep). following once daily dosing of 10 mg, the mean treatment difference (dayvigo – placebo) on day 8 for the apnea-hypopnea index was -0.80 (95% ci: -4.88 to 3.29). due to study limitations, including the short duration of the study, clinically meaningful respiratory effects of dayvigo in osa cannot be excluded, including for long-term treatment [see warnings and precautions ( 5.4 )] . chronic obstructive pulmonary disease (copd) the respiratory depressant effect of dayvigo was evaluated after 8 consecutive nights of treatment with dayvigo 10 mg in a randomized, placebo-controlled, two-period crossover study in 30 patients with moderate to severe copd (forced expiratory volume in the first second (fev1 )/forced vital capacity (fvc) ratio ≤ 70% and 30% ≤ fev1 < 80% of predicted). following once-daily dosing of 10 mg, the mean treatment difference (dayvigo – placebo) on day 8 for the mean peripheral capillary oxygen saturation during sleep was 0.47 (95% ci: 0.07 to 0.87). dayvigo has not been studied in copd patients with a fev1 < 30% of predicted. clinically meaningful respiratory effects of dayvigo in patients with compromised respiratory function cannot be excluded [see warnings and precautions ( 5.4 )] . dayvigo contains lemborexant, a schedule iv controlled substance. abuse is the intentional, non-therapeutic use of a drug, even once, for its desirable psychological or physiological effects. in a human abuse potential study conducted in recreational sedative abusers (n=29), lemborexant 10 mg, 20 mg (two times the maximum recommended dose), and 30 mg (three times the maximum recommended dose) produced responses on positive subjective measures such as “drug liking,” “overall drug liking,” “take drug again,” and “good drug effects” that were statistically similar to those produced by the sedatives zolpidem (30 mg) and suvorexant (40 mg), and statistically greater than the responses on these measures that were produced by placebo. because individuals with a history of abuse or addiction to alcohol or other drugs may be at increased risk for abuse and addiction to dayvigo, follow such patients carefully. physical dependence is a state that develops as a result of physiological adaptation in response to repeated drug use, manifested by withdrawal signs and symptoms after abrupt discontinuation or a significant dose reduction of a drug. in animal studies and clinical trials evaluating physical dependence, chronic administration of lemborexant did not produce withdrawal signs or symptoms upon drug discontinuation. this suggests that lemborexant does not produce physical dependence.