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Dosage adjustment for patients with impaired renal function on the basis of experience with a group of subjects with severely impaired renal function treated with ranitidine, the recommended dosage in patients with a creatinine clearance 50 ml min is 150 mg every 24 hours and remeron. Patients have been described with galactorrhea associated with sustained hyperprolactinemia due to verapamil.77, 78 In a survey of patients taking verapamil in an outpatient clinic, PRL levels were elevated in 8.5% of patients, 79 and hyperprolactinemia was associated with lower testosterone levels. Verapamil is believed to cause hyperprolactinemia by blocking the hypothalamic generation of dopamine.75, 76 Other calcium channel blockers such as the dihydropyridines and benzothiazepines have no action on PRL secretion.76 -Methyldopa causes moderate hyperprolactinemia, possibly by inhibiting the enzyme aromatic-L-amino-acid decarboxylase, which is responsible for converting L-dopa to dopamine, and by acting as a false neurotransmitter to decrease dopamine synthesis.80 Reserpine, a little-used antihypertensive drug, causes hyperprolactinemia in about 50% of patients, likely by interfering with the storage of hypothalamic catecholamines in secretory granules.81 Enalapril, an angiotensin-converting enzyme inhibitor, inhibits PRL release in some individuals, 82 but sustained alterations of PRL levels have not been reported with use of this class of medications. GASTROINTESTINAL MEDICATIONS Two drugs commonly used to increase gastrointestinal motility and stomach emptying in patients with gastroparesis diabeticorum, metoclopramide and domperidone, are dopamine receptor blockers. These drugs cause hyperprolactinemia in more than 50% of patients and commonly cause symptoms of amenorrhea and galactorrhea in women and impotence in men.83-85 Another drug used for this purpose, cisapride, does not block dopamine receptors and does not cause hyperprolactinemia. At present in the United States, only metoclopramide is available for this use, but the other drugs are available in many other countries. Chlorpromazine, a commonly used antinausea drug, is a phenothiazine and causes acute hyperprolactinemia6; however, it is not commonly used long-term. Shortly after the approval of histamine2 receptor blockers such as cimetidine and ranitidine, several brief case reports were published about patients experiencing symptoms related to hyperprolactinemia.86, 87 However, in larger series, hyperprolactinemia has not been reported, and there have been no subsequent reports of hyperprolactinemia occurring with this class of drugs88-91 except for 1 case of a woman treated with a twice-maximum dose of famotidine.92 PROTEASE INHIBITORS In 2000, Hutchinson et al93 described 4 patients who were hyperprolactinemic while receiving protease inhibitors as part of highly active antiretroviral therapy or prophylactic.

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LBBC is partnering with researchers to study the needs of women who are five or more years past a breast cancer diagnosis. Julie Becker, PhD, MPH, of Thomas Jefferson University, and Andrea CrivelliKovach, PhD, CHES, of Arcadia University, conducted several focus groups of women in the Philadelphia area, including many women involved with LBBC. The researchers' goal is to understand how women who have passed the five-year survival mark think about their health and seek health information. The researchers will use the information to study whether women could benefit from a program to help them manage symptoms or prevent additional cancers or other chronic diseases. Funding for "Health Information Seeking Behavior of Long-Term Breast Cancer Survivors Using a Self-Management Model" came from the state of Pennsylvania. Drs. Becker and Crivelli-Kovach received a one-year grant including LBBC as a partner in recruiting participants. Focus groups were held in diverse Philadelphia-area neighborhoods with women ages 40-66 who are five years past diagnosis without a recurrence or an unrelated cancer. The self-management model will be piloted in early spring 2006. To learn more, please contact Abbie Schlener at 215.955.7713 or and ritalin.
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Options designs and arranges technical briefing programmes for DFID staff who are new to current reproductive health issues. Recently, we organised such a programme for Jean Lennock, the new DFID Deputy Health and Population Field Manager in Lagos, Nigeria. This included a week of technical briefings with experts in the fields of adolescent sexual health, STD HIV and AIDS, malaria and safe motherhood. We also arranged visits to organisations active in reproductive and sexual health, including AHRTAG, International Family Health, Centre for International Child Health, IPPF, London School of Hygiene and Tropical Medicine and the UK NGO AIDS Consortium. Contact: Katie Chapman and singulair.

1. Arky R et al: Physicians' desk reference. Medical Economics Company, Montvale, 1998; pp 528-532 2. Goves J, Oldring JK, Kerr D et al: First line treatment with omeprazole provides an effective and superior alternative strategy in the management of dyspepsia compared to antacid alginate liquid: a multicentre study in general practice. Aliment Phamacol Ther, 1998; 12: 147-157 Carlsson E, Larsson E, Mattsson H et al: Pharmacology and toxicology of omeprazole with special references to the effects on the gastric mucosa. Scand J Gastroenterol, 1986; 118 Suppl ; : 31-38 4. Pinson DM, Havu N, Sztern MI et al: Drug-inducted hypergastrinemia: absence of trophic effects on colonic carcinoma in rats. Gastroenterology, 1995; 108: 1068-1074 Mereto E, Ghia M, Martelii A, Brambilla G: Lack of evidence of omeprazole genotoxicity in Sprague-Daweley rats. Mutagenesis, 1993; 8: 379-386 Bartosz G: Druga twarz tlenu. PWN, Warsaw, 1995 7. Ledwoyw A: The relationship between plasma triglycerides, cholesterol, total lipids and lipid peroxidation products during human atherosclerosis. Clin Chim Acta, 1986; 155: 275-283 Lowry OH, Rosenbrough NI, Farr AL, Randall RJ: Protein measurement with the Fohlin phenol reagent. J Biol Chem 1951; 193: 265-275 Hahm KB, Lee KJ, Kim YS et al: Augmented eradication rates of Helicobacter pylori by new combination therapy with lansoprazole, amoxicillin, and rebamipide. Dig Dis Sci, 1998; 43: 235-240 Powers RE, Lawton GP, Modlin IM: Genotoxicity, Carcinogenicity and acid suppressing medications. Pharmacol Ther, 1995; 65: 303-317 Betton GR, Dormer CS, Wells T et al: Gastric ECL-cell hyperplasia and carcinoids in rodents following chronic administration of H2antagonists SK&F; 93479 and oxmetidine and omeprazole. Toxicol Pathol, 1988; 16, 288-298 Havu N: Enterochromaffin-like cell carcinoid of gastric mucosa in rats after life-long inhibition of gastric acid secretion. Digestion, 1986; 35 Suppl 1 ; : 42-55 13. Larsson H, Carlsson E, Mattsson H et al: Plasma gastrin and gastric enterochromaffin like cell activation and proliferation. Studies with omeprazole and ranitidine in intact and antrectomized rats. Gastroenterology, 1988; 90: 391-399.
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Richter JE. Gastroesophageal reflux disease in the older patient: presentation, treatment, and complications. J Gastroenterol. 2000; 95: 368-373. Raiha IJ, Impivaara O, Seppala M, Sourander LB. Prevalence and characteristics of symptomatic gastroesophageal reflux disease in the elderly. J Geriatr Soc. 1992; 40: 1209-1211. Lagergren J, Bergstrom R, Lindgren A, Nyren O. Symptomatic gastroesophageal reflux as a risk factor for esophageal adenocarcinoma. N Engl J Med. 1999; 340: 825-831. Locke GR III, Talley NJ, Fett SL, Zinsmeister AR, Melton LJ III. Prevalence and clinical spectrum of gastroesophageal reflux: a population-based study in Olmsted County, Minnesota. Gastroenterology. 1997; 112: 1448-1456. Richter JE. Long-term management of gastroesophageal reflux disease and its complications. J Gastroenterol. 1997; 92 4, suppl ; : 30S-34S. Katz PO. Treatment of gastroesophageal reflux disease: use of algorithms to aid in management. J Gastroenterol. 1999; 94 11, suppl ; : S3-S10. Sonnenberg A, Steinkamp U, Weise A, et al. Salivary secretion in reflux esophagitis. Gastroenterology. 1982; 83: 889-895. Piotrowski J. Saliva and esophagoprotection [letter]. Gastroenterology. 1996; 111: 834-837. Holloway R, Dent J. Pathophysiology of gastroesophageal reflux: lower esophageal sphincter dysfunction in gastroesophageal disease. Gastroenterol Clin North Am. 1990; 19: 517-535. Mittal RK, Holloway RH, Penagini R, Blackshaw LA, Dent J. Transient lower esophageal sphincter relaxation. Gastroenterology. 1995; 109: 601-610. Hinder RA, Smith SL, Klingler PJ, Branton SA, Floch NR, Seelig MH. Laparoscopic antireflux surgery--it's a wrap. Dig Surg. 1999; 16: 7-11. Morales TG, Sampliner RE. Barrett's esophagus: update on screening, surveillance, and treatment. Arch Intern Med. 1999; 159: 14111416. Harris RA, Kuppermann M, Richter JE. Prevention of recurrences of erosive reflux esophagitis: a cost-effectiveness analysis of maintenance proton pump inhibition. J Med. 1997; 102: 78-88. DeVault KR. Overview of medical therapy for gastroesophageal reflux disease. Gastroenterol Clin North Am. 1999; 28: 831-845. Hamilton JW, Boisen RJ, Yamamoto DT, Wagner JL, Reichelderfer M. Sleeping on a wedge diminishes exposure of the esophagus to refluxed acid. Dig Dis Sci. 1988; 33: 518-522. DeVault KR, Castell DO, Practice Parameters Committee of the American College of Gastroenterology. Updated guidelines for the diagnosis and treatment of gastroesophageal reflux disease. J Gastroenterol. 1999; 94: 1434-1442. Wolfe MM, Sachs G. Acid suppression: optimizing therapy for gastroduodenal ulcer healing, gastroesophageal reflux disease, and stress-related erosive syndrome. Gastroenterology. 2000; 118 suppl ; : S9-S31. Sontag SJ. The medical management of reflux esophagitis: role of antacids and acid inhibition. Gastroenterol Clin North Am. 1990; 19: 683-712. Castell DO, Sigmund C Jr, Patterson D, et al, CIS-USA-52 Investigator Group. Cisapride 20 mg b.i.d. provides symptomatic relief of heartburn and related symptoms of chronic mild to moderate gastroesophageal reflux disease. J Gastroenterol. 1998; 93: 547552. Castell D. My approach to the difficult GERD patient. Eur J Gastroenterol Hepatol. 1999; 11 suppl 1 ; : S17-S23. Williams CN. An important drug interaction. Can J Gastroenterol. 1998; 12: 535. Piquette RK. Torsade de pointes induced by cisapride clarithromycin interaction. Ann Pharmacother. 1999; 33: 22-26. Bardhan KD, Muller-Lissner S, Bigard MA, et al, European Study Group. Symptomatic gastro-oesophageal reflux disease: double blind controlled study of intermittent treatment with omeprazole or ranitidine. BMJ. 1999; 318: 502-507.

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Many americans believe they control nature to meet their needs and thus are more likely to seek health care when needed. Now required to enable accurate species identification of the nonpigmented and late-pigmenting RGM Tables 3 and 4 ; . Although highly accurate at identifying slowly growing nontuberculous mycobacteria to species, HPLC has proven to be ineffective in identifying these organisms to the species level. Biochemical and Phenotypic Identification After establishing a clinical isolate as an RGM, the best combination of traditional tests for recognition of the most commonly encountered species include the 3-day arylsulfatase test, iron uptake, nitrate reductase, and utilization of the carbohydrates mannitol, inositol, and citrate Table 4 ; . A number of additional nonmolecular tests have also been utilized. A disk diffusion test using polymyxin B can also distinguish between the M. fortuitum group and the M. chelonae-abscessus group. Isolates of the M. fortuitum group exhibit a partial or complete zone of growth inhibition of 10 mm greater around the polymyxin disk, whereas isolates of the M. chelonae-abscessus group show no partial or complete zone of inhibition 204 ; . A previous IWGMT study 86 ; showed that growth in 5% NaCl could reliably differentiate strains of M. abscessus 100% positive ; from M. chelonae 17% positive ; . The citrate test was also found to be another useful biochemical test in that approximately 80% of M. abscessus isolates were citrate negative and 100% of M. chelonae isolates were citrate positive 86 ; . In our hands, the citrate utilization test has proven highly reliable. ; Additionally, of the M. fortuitum group, only the unnamed third biovariant complex is positive for inositol. Utilizing molecular methods as the standard of identification, positive citrate tests with M. abscessus are rare 219, for example, ranitidine bismuth citrate. 2826. Hertzog JH, Campbell JK, Dalton HJ, et al. Propofol anesthesia for invasive procedures in ambulatory and hospitalized children: experience in the pediatric intensive care unit. Pediatrics. 1999; 103 3 ; . Available at: : pediatrics cgi content full 103 3 e30. 2827. Rigby-Jones AE, Nolan JA, Priston MJ, et al. Pharmacokinetics of propofol infusions in critically ill neonates, infants, and children in an intensive care unit. Anesthesiol. 2002; 97: 13931400. Cornfield DN, Tegtmeyer K, Nelson MD, et al. Continuous propofol infusion in 142 critically ill children. Pediatrics. 2002; 110: 11771181. Cray SH, Robinson BH, Cox PN. Lactic academia and bradyarrhythmia in a child sedated with propofol. Crit Care Med. 1998; 26: 20872092. Wolf A, Weir P, Segar P, et al. Imparied fatty acid oxidation in propofol infusion syndrome. Lancet. 2001; 357: 606607. Boigner H, Lechner E, Brock H, et al. Life threatening cardiopulmonary failure in an infant following protamine reversal of heparin after cardiopulmonary bypass. Paediatr Anaesth. 2001; 11: 729732. Lugo RA, Harrison M, Cash J, et al. Pharmacokinetics and pharmacodynamics of ranitidine in critically ill children. Crit Care Med. 2001; 29: 759764. Staatz CE, Taylor PJ, Lynch SV, et al. Population pharmacokinetics of tacrolimus in children who receive cut-down or full liver transplants. Transplantation. 2001; 72: 10561061 and relafen. Members take advantage of the NC HealthSmart initiative in many different ways. Listed below are just some of the ways members like you have used the initiative. Remember, all of these services are free. Back & Neck Pain "I went to the Back and Neck Pain Condition Center and filled out a very easy survey. I received tips on how to manage my pain." Join the thousands of other NC HealthSmart members who have taken their Health Risk Assessment HRA ; --a simple survey that allows you to better manage your health. Talk to a Health Coach about any health concern you or a family member may be experiencing. You can call as often as you like. Create a 13 week personal exercise plan that allows you to track your progress. Go to: shpnc Click on the NC HealthSmart link Log into your Personal Health Portal Click on the Back and Neck Condition Center for more information Go to: shpnc Click on the NC HealthSmart link Log into your Personal Health Portal Take your HRA Call 1-800-817-7044 24 hours a day, 7 days a week.
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