Ranitidine (Page 2 of 5)

2. Effects on Other Gastrointestinal Secretions

Pepsin

Ranitidine does not affect pepsin secretion. Total pepsin output is reduced in proportion to the decrease in volume of gastric juice.

Intrinsic Factor

Ranitidine has no significant effect on pentagastrin-stimulated intrinsic factor secretion.

Serum Gastrin

Ranitidine has little or no effect on fasting or postprandial serum gastrin.

Other Pharmacologic Actions

a. Gastric bacterial flora – increase in nitrate-reducing organisms, significance not known.
b. Prolactin levels – no effect in recommended dosage.
c. Other pituitary hormones – no effect on serum gonadotropins, TSH, or GH. Possible impairment of vasopressin release.
d. No change in cortisol, aldosterone, androgen, or estrogen levels.
e. No antiandrogenic action.f. No effect on count, motility, or morphology of sperm.

Pediatrics

Oral doses of 6 mg/kg to 10 mg/kg per day in two or three divided doses maintain gastric pH > 4 throughout most of the dosing interval.

Clinical Trials

Active Duodenal Ulcer

In a multicenter, double-blind, controlled, US study of endoscopically diagnosed duodenal ulcers, earlier healing was seen in the patients treated with ranitidine as shown in Table 3.

Table 3: Duodenal Ulcer Patient Healing Rates
* All patients were permitted antacids as needed for relief of pain. P <0.0001.
Ranitidine* Placebo*
Number Entered Healed/ Evaluable Number Entered Healed/ Evaluable
OutpatientsWeek 2 195 69/182 188 31/164
(38%) (19%)
Week 4 137/187 76/168
(73%) (45%)

In these studies, patients treated with ranitidine reported a reduction in both daytime and nocturnal pain, and they also consumed less antacid than the placebo-treated patients.

Table 4: Mean Daily Doses of Antacid
Ulcer Healed Ulcer Not Healed
Ranitidine 0.06 0.71
Placebo 0.71 1.43

Foreign studies have shown that patients heal equally well with 150 mg two times a day and 300 mg at bedtime (85% versus 84%, respectively) during a usual 4-week course of therapy. If patients require extended therapy of 8 weeks, the healing rate may be higher for 150 mg two times a day as compared to 300 mg at bedtime (92% versus 87%, respectively).

Studies have been limited to short-term treatment of acute duodenal ulcer. Patients whose ulcers healed during therapy had recurrences of ulcers at the usual rates.

Maintenance Therapy in Duodenal Ulcer

Ranitidine has been found to be effective as maintenance therapy for patients following healing of acute duodenal ulcers. In two independent, double-blind, multicenter, controlled trials, the number of duodenal ulcers observed was significantly less in patients treated with ranitidine (150 mg at bedtime) than in patients treated with placebo over a 12-month period.

Table 5: Duodenal Ulcer Prevalence
* RAN = ranitidine. % = Life Table estimate. P <0.05 (Ranitidine versus comparator)§ PLC = placebo.
Double-blind, Multicenter, Placebo-Controlled Trials
Multicenter Trial Drug Duodenal Ulcer Prevalence No. of Patients
0-4 Months 0-8 Months 0-12 Months
RAN * 20% 24% 35% 138
USA PLC § 44% 54% 59% 139
RAN* 12% 21% 28% 174
Foreign PLC§ 56% 64% 68% 165

As with other H2 -antagonists, the factors responsible for the significant reduction in the prevalence of duodenal ulcers include prevention of recurrence of ulcers, more rapid healing of ulcers that may occur during maintenance therapy, or both.

Gastric Ulcer

In a multicenter, double-blind, controlled, US study of endoscopically diagnosed gastric ulcers, earlier healing was seen in the patients treated with ranitidine as shown in Table 6.

Table 6: Gastric Ulcer Patient Healing Rates
* All patients were permitted antacids as needed for relief of pain. P =0.009 .
Ranitidine* Placebo*
Number Entered Healed/ Evaluable Number Entered Healed/ Evaluable
OutpatientsWeek 2 92 16/83 94 10/83
(19%) (12%)
Week 6 50/73 35/69
(68%) (51%)

In this multicenter trial, significantly more patients treated with ranitidine became pain free during therapy.

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