uld be used with extreme caution in patients having an acute asthmatic attack, patients with chronic obstructive pulmonary disease or cor pulmonale, patients having a substantially decreased respiratory reserve and patients with pre-existing respiratory depression, hypoxia or hypercapnia. in such patients, even usual therapeutic doses of narcotics may decrease respiratory drive while simultaneously increasing airway resistance to the point of apnea. intravenous use if necessary, hydromorphone may be given intravenously, but the injection should be given very slowly (over a period of at least 3 to 5 minutes). rapid intravenous injection of narcotic analgesics, including hydromorphone, increases the incidence of adverse reactions; severe respiratory depression, apnea, hypotension, peripheral circulatory collapse, cardiac arrest, as well as anaphylactoid reactions, have occurred. hydromorphone should not be administered intravenously unless a narcotic antagonist and the facilities for resuscitation and assisted or controlled respiration are immediately available. when hydromorphone is given parenterally, especially intravenously, the patient should be lying down. hypotensive effect the administration of hydromorphone may result in severe hypotension in an individual whose ability to maintain blood pressure has already been compromised by a depleted blood volume or concurrent administration of drugs such as the phenothiazines or certain anesthetics. hydromorphone may produce orthostatic hypotension in ambulatory patients.

hydromorphone is used postoperatively and in patients with pulmonary disease.

tainer permit.

xperience increased colonic motility; in patients with acute ulcerative colitis, toxic dilatation has been reported with narcotics. cardiovascular system: circulatory depression, peripheral circulatory collapse and cardiac arrest have occurred after rapid intravenous injection. orthostatic hypotension and fainting may occur, especially if a patient stands up suddenly after receiving an injection of hydromorphone. additionally, hydromorphone may cause tachycardia, bradycardia and palpitations. genitourinary system: oliguria, ureteral spasm, spasm of vesical sphincters and urinary retention have been reported. respiratory depression: hydromorphone produces dose-related respiratory depression by acting directly on brain stem respiratory centers. hydromorphone also affects centers that control respiratory rhythm and may produce irregular and periodic breathing. if significant respiratory depression occurs, it may be antagonized by the use of naloxone hydrochloride. in patients who are physically dependent, small doses of naloxone may be sufficient not only to antagonize respiratory depression but also to precipitate withdrawal phenomena. the dose of naloxone should, therefore, be adjusted accordingly in such patients. since the duration of action of hydromorphone may exceed that of the antagonist, the patient should be kept under continued surveillance; repeated doses of the antagonist may be required to maintain adequate respiration. apply other supportive measures when indicated. allergic: allergic reactions to opiates occur infrequently; pruritus, urticaria and other skin rashes are most common. anaphylactoid reactions have been reported following intravenous administration of opiates. other: opiate-induced histamine release may be responsible for the flushing of the face, sweating and pruritus often seen with these drugs. wheals and urticaria at the site of injection are probably related to histamine release. local tissue irritation, pain and induration have been reported following repeated subcutaneous injection.

dvantage in the postoperative period, since the patient with a less-clouded sensorium is better able to cooperate in early ambulation procedures. likewise, cancer patients can be relieved of pain yet remain sufficiently alert to function within the scope of their underlying physical disorder. narcotic analgesics also depress various respiratory centers, depress the cough reflex, constrict the pupils, elevate cerebrospinal fluid pressure, produce transient hyperglycemia and enhance parasympathetic activity. narcotic analgesics may cause nausea and vomiting by stimulating the chemoreceptor trigger zone (ctz); however, they also depress the vomiting center, so that subsequent doses are unlikely to produce vomiting. nausea and vomiting are significantly more common in ambulatory than in recumbent patients. narcotic analgesics, including hydromorphone, increase the tone and decrease the propulsive contractions of the smooth muscle of the gastrointestinal tract. the resultant prolongation in gastrointestinal transit time is responsible for hydromorphone’s constipating effect. because narcotics may increase biliary tract pressure, some patients with biliary colic may experience worsening rather than relief of pain. while narcotics generally increase the tone of urinary tract smooth muscle, the net effect tends to be variable, in some cases producing urinary urgency, in others, difficulty in urination. narcotics have also been reported to cause antidiuretic hormone (adh) to be released, thereby reducing urine output. in therapeutic dosage, opiates do not usually exert major effects on the cardiovascular system. however, some patients exhibit a propensity to develop orthostatic hypotension and fainting. rapid intravenous injection is more likely to precipitate a fall in blood pressure than are intramuscular or subcutaneous injections. narcotic analgesics cause histamine release, which appears to be responsible for wheals or urticaria sometimes seen at the site of injection. histamine release may also produce dilation of cutaneous blood vessels, with resultant flushing of the face and neck, pruritus and sweating. hydromorphone is well absorbed after parenteral administration. after intramuscular administration, hydromorphone has a slightly more rapid onset and slightly shorter duration of analgesia than morphine. the major pathway of hydromorphone metabolism is conjugation with glucuronic acid in the liver; hydromorphone glucuronide is excreted primarily in the urine.