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Isotonic Infusion Solution for Intravenous Administration
Indication
1. Substitution of fluid losses, imbalanced acid-base equilibrium and slight acidosis.
2. Primary volume substitution in emergency cases.
3. Used in cases of dehydration, sodium depletion, repletion of gastrointestinal loss and in metabolic acidosis syndromes.
Contraindication:
§ Hypernatraemia,
§ Renal imsufficiency,
§ Liver cell damage,
§ Lactic acidosis,
Note: Not for treatment of lactic acidosis.
Precautions:
Do not use if leakage was found, solution is cloudy or contains particles.
Intravenous infusion: Max. 3 ml/kg BW/hr.
1000 ml/70 kg BW/day up to 7.0 ml/kg BW.
NA
Store below 25° C.
Each 100 ml contains:
Sodium Chloride | 0.86 g |
Potassium Chloride | 0.03 g |
Calcium Chloride 2H2O | 0.033 g |
Water for Injection | Q.S. |
(mEq/L): Na+ (147) K+ (4) Ca++ (4.5) Cl¯ (155.5) | |
pH | 5.0 – 7.5 |
Theor. Osmolarity | 311 mOsm/L |
Kuwait Saudi Pharmaceutical Industries Company
Tel: +965 24745012/3/4
Fax: +965 24745361, P. O. Box: 5512, postal code: 13056 Safat, Kuwait
Website: www.kspico.com
محلول رينجرز للحقن الوريدي (ي س ف)
١. كمحلول معوض في حالات فقد السوائل، حالات عدم الاتزان الحمضي القاعدي أو عند الحموضة البسيطة للدم.
۲. كمحلول حجمي معوض أساسي في حالات الطوارئ.
۳. كمحلول معوض في حالات نقص الصوديوم و الأملاح.
§ حالات ارتفاع الصوديوم في الدم،
§ الفشل الكلوي،
§ تأثر خلايا الكبد،
§ ارتفاع حموضة الدم نتيجة زيادة معدل حمض اللاكتيك،
ملاحظة: لا يستخدم لعلاج هذه الحالة.
لا تستعمله إن وجد تسريب، أو إذا كان المحلول معكر أو يحتوي على شوائب.
عن طريق الحقن الوريدي:
۳ مل/ كجم من وزن الجسم/ ساعة
أي ١۰۰۰ مل/ ٧۰ كجم من وزن الجسم/ يوم أو حتى ٧ مل/ كجم من وزن الجسم/.
۲١۰ مل/ ساعة/ ٧۰ كجم من وزن الجسم.
غير متاح
يحفظ في درجة حرارة أقل من ٢٥ درجة مئوية.
الشكل الصيدلي |
محلول للحقن الوريدي متعادل الضغط الاسموزي
التركيب |
يحتوي كل ١۰۰ مل من المحلول على:
صوديوم كلوريد | ۰,٨٦ جم |
بوتاسيوم كلوريد | ۰,۰۳ جم |
كالسيوم كلوريد ثنائي مائي | ۰,۰۳۳ جم |
ماء للحقن | بقية المحلول |
يحتوي كل ١۰۰۰ مل من المحلول على (ميلي مكافئ): |
|
صوديوم (١٤٧)، بوتاسيوم (٤)، كالسيوم (٤,٥)، كلوريد (١٥٥,٥) |
|
الأس الهيدروجيني (معدل الحموضة) | ٥,۰ – ٧,٥ |
الضغط الأسموزي الافتراضي | ۳١١ ملي أوزم/ لتر |
الشكل الصيدلي |
محلول للحقن الوريدي متعادل الضغط الاسموزي
الشركة المصنعة والمفوضة بالتسويق
الشركة الكويتية السعودية للصناعات الدوائيه
ص ب: 5512 ،الرمز البريدي: 13056 الصفاة، الكويت
هاتف: 96524745013-96524745014+
فاكس: 96524745361+
الموقع الالكتروني: www.kspico.com
Ringer's Injection U.S.P. is indicated to:
- Replace extracellular fluid losses,
- Restore the sodium, potassium, calcium and chloride balances, for treatment of isotonic dehydration
POSOLOGY
Adults, the Elderly, Adolescents and Children:
The dosage depends on the age, weight, clinical and biological conditions of the patient and concomitant therapy.
Recommended dosage:
The recommended dosage is:
- for adults, the elderly and adolescents : 500 ml to 3 litres /24h
- for babies and children : 20 ml to 100 ml / kg / 24 h.
Administration rate:
The infusion rate is usually 40 ml/kg/24h in adults, the elderly and adolescents.
In paediatric patients the infusion rate is 5 ml/kg/h on average but the value varies with age: 6-8 ml/kg/h for infants, 4-6 ml/kg/h for toddlers, and 2-4 ml/kg/h for schoolchildren. In children with burns, the dose is on average 3.4 ml/kg/per cent burn at 24 h post-burn and 6.3 ml/kg/per cent burn at 48 h.
In severely head-injured children the dose is on average 2850 ml/m2.
Infusion rate and total volume can be higher in surgery or in case of need.
Note:
- infants and toddlers: aged from 28 days to 23 months (a toddler is an infant who can walk)
- children and schoolchildren: aged from 2 years to 11 years.
METHOD OF ADMINISTRATION:
The administration is performed by intravenous route.
The solution for infusion should be visually inspected prior to use.
Use only if the solution is clear, without visible particles and if the container is undamaged. Administer immediately following the insertion of infusion set.
Do not use plastic containers in series connections. Such use could result in air embolism due to residual air being drawn from the primary container before the administration of the fluid from the secondary container is completed.
Pressurizing intravenous solutions contained in flexible plastic containers to increase flow rates can result in air embolism if the residual air in the container is not fully evacuated prior to administration.
Use of a vented intravenous administration set with the vent in the open position could result in air embolism. Vented intravenous administration sets with the vent in the open position should not be used with flexible plastic containers.
The solution should be administered with sterile equipment using an aseptic technique. The equipment should be primed with the solution in order to prevent air entering the system.
Additives may be introduced before infusion or during infusion through the injection site.
MONITORING
Fluid balance and plasma electrolytes concentrations (sodium, potassium, calcium and chlorides) must be monitored during administration.
Cases of fatal reactions with calcium-ceftriaxone precipitates in lungs and kidneys in premature and full-term newborn infants aged less than 1 month have been described.
In patients of any age ceftriaxone must not be mixed or administered simultaneously with any calcium-containing IV solutions even via different infusion lines or different infusion sites
However, in patients older than 28 days of age ceftriaxone and calcium-containing solutions may be administered sequentially one after another if infusion lines at different sites are used or if the infusion lines are replaced or thoroughly flushed between infusions with physiological salt-solution to avoid precipitation. Sequential infusions of ceftriaxone and calcium-containing products must be avoided in case of hypovolaemia.
High volume infusion must be used under specific monitoring in patients with cardiac or pulmonary failure.
Solutions containing sodium chloride should be administered with caution to patients with hypertension, heart failure, peripheral or pulmonary oedema, impaired renal function, pre-eclampsia, aldosteronism or other conditions or treatment (e.g. corticoids/steroids) associated with sodium retention (see also Section 4.5 – Interactions with other medicinal products and other forms of interaction).
Solutions containing potassium salts should be administered with caution to patients with cardiac disease, or conditions predisposing to hyperkalemia such as renal or adrenocortical insufficiency, acute dehydration, or extensive tissue destruction as occurs with severe burns.
Because of the presence of calcium:
- care should be taken to prevent extravasation during intravenous infusion
- the solution should be given cautiously to patients with impaired renal function or diseases associated with elevated vitamin D concentrations such as sarcoidosis
- in case of concomitant blood transfusion, the solution must not be administered via the same infusion set because of the risk of coagulation.
Ringer's Injection U.S.P. contains insufficient concentration of potassium and calcium to be used for maintenance of these ions or to correct their deficits. Hence, after dehydration is treated, the IV fluid has to be changed to a maintenance fluid that will provide these ions.
During long-term parenteral treatment, a convenient nutritive supply must be given to the patient.
For information on preparation of the product and additives, please see section 6.6.
Interaction with ceftriaxone
- Concomitant treatment with ceftriaxone and Ringer's Injection U.S.P. is contraindicated in preterm newborn infants and term newborn infants (≤28 days of age), even if separate infusion lines are used (risk of fatal ceftriaxone-calcium salt precipitation in the neonate's bloodstream) (see Section 4.3).
- In patients older than 28 days (including adults), ceftriaxone must not be administered simultaneously with intravenous calcium-containing solutions, including Ringer's Injection U.S.P. (See Section 4.4) even via different infusion lines or different infusion sites (see section 6.2).
Interaction related to the presence of sodium:
- Corticoids/Steroids and carbenoxolone, which are associated with the retention of sodium and water (with oedema and hypertension).
Interaction related to the presence of potassium:
- Potassium-sparing diuretics (amiloride, spironolactone, triamterene, alone or in association),
- Angiotensin converting enzyme inhibitors (ACEI) and, by extrapolation, angiotensin II receptor antagonists
- Tacrolimus, cyclosporine which increase concentration of potassium in the plasma and may lead to potentially fatal hyperkalaemia notably in case of a renal failure increasing the hyperkalaemic effect
Interaction related to the presence of calcium:
- Digitalis glycosides (digitalis cardiotonics) whose effects are enhanced by the presence of calcium and may lead to serious or fatal cardiac arrhythmia
- Thiazide diuretics or vitamin D which can lead to hypercalcaemia when co-administered with calcium.
For information on incompatibilities between this and other products, please see section 6.2.
Ringer's Injection U.S.P. can be used safely during pregnancy and lactation as long as the electrolyte and fluid balance is controlled.
When a medicinal product is added, the nature of the drug and its use during pregnancy and lactation have to be considered separately.
Not relevant.
During administration of Ringer's Injection, the adverse reactions have been reported as very common (≥ 10%):
- Hyperhydration and heart failure in patients with cardiac disorder or pulmonary oedema
- Electrolytes disturbances.
Adverse reactions may be associated to the technique of administration including febrile response, infection at the site of injection, local pain or reaction, vein irritation, venous thrombosis or phlebitis extending from the site of injection and extravasation.
Adverse reactions may be associated to the medicinal product added to the solution; the nature of the additive will determine the likelihood of any other adverse reactions.
In case of adverse reaction(s), the infusion must be discontinued.
To report any side effect(s):
Saudi Arabia, Saudi Food & Drug Authority: National Pharmacovigilance Center To contact Executive Administration for Pharmacovigilance & Crisis Management. Tel: +966-11-203-8222 ext 2340-2317-2356 Hotline: 19999 FAX: +966112057662 E-MAIL: npc.drug@sfda.gov.sa WEBSITE: www.sfda.gov.sa/npc |
Overdose or too fast administration may lead to water and sodium overload with a risk of oedema, particularly when there is a defective renal sodium excretion. In this case extra renal dialysis may be necessary.
Excessive administration of potassium may lead to the development of hyperkalaemia, especially in patients with renal impairment. Symptoms include paresthesia of the extremities, muscle weakness, paralysis, cardiac arrhythmias, heart block, cardiac arrest, and mental confusion.
Treatment of hyperkalaemia involves the administration of calcium, insulin (with glucose), sodium bicarbonate, exchange resins or dialysis.
Excessive administration of calcium salts may lead to hypercalaemia. Symptoms of hypercalaemia may include anorexia, nausea, vomiting, constipation, abdominal pain, muscle weakness, mental disturbances, polydipsia, polyuria, nephrocalcinosis, renal calculi, and, in severe cases, cardiac arrhythmias and coma. Too rapid intravenous injection of calcium salts may also lead to many of the symptoms of hypercalaemia as well as to a chalky taste, hot flushes, and peripheral vasodilatation. Mild asymptomatic hypercalaemia will usually resolve on stopping administration of calcium and other contributory drugs such as vitamin D. If hypercalaemia is severe, urgent treatment (such as loop diuretics, haemodialysis, calcitonin, bisphosphonates, trisodium edetate) is required.
Excessive administration of chloride salts may cause a loss of bicarbonate with an acidifying effect.
When overdose is related to medicinal products added to the solution infused, the signs and symptoms of over infusion will be related to the nature of the additive being used.
In the event of accidental over infusion, treatment should be discontinued and the patient should be observed for the appropriate signs and symptoms related to the drug administered. The relevant symptomatic and supportive measures should be provided as necessary.
Pharmacotherapeutic group: “ Electrolytes”, ATC code: "B05BB01”
Ringer's Injection U.S.P. is an isotonic solution of electrolytes. The constituents of Ringer's Injection U.S.P. and their concentrations are designed to match those of plasma.
The pharmacodynamic properties of this solution are those of its components (water, sodium, potassium, calcium, and chloride). The main effect of Ringer's Injection U.S.P. is the expansion of the extracellular compartment including both the interstitial and intravascular fluids.
Ions, such as sodium, circulate through the cell membrane using various mechanisms of transport among which is the sodium pump (Na+/K+-ATPase). Sodium plays an important role in neurotransmission and cardiac electrophysiology, and also in its renal metabolism.
Potassium is essential for numerous metabolic and physiological processes including nerve conduction, muscle contraction, and acid-base regulation. A normal concentration of potassium in plasma is about 3.5 to 5.0 mmoles per litre. Potassium is predominantly an intracellular cation, primarily found in muscle; only about 2% is present in the extracellular fluid. The passage of potassium into the cells and retention against the concentration gradient requires active transport via the Na+/K+-ATPase enzyme.
Approximately 99% of calcium is incorporated into the skeleton. The remaining 1% is found in body tissues and fluids, and is essential for normal nerve conduction, muscle activity, and blood coagulation.
Chloride is mainly an extracellular anion found in low concentration in bone and in high concentration in some components of connective tissue such as collagen. Intracellular chloride is in high concentration in red blood cells and gastric mucosa. The balance of anions and cations are regulated by the kidneys. Reabsorption of chloride generally follows reabsorption of sodium.
The pharmacokinetic properties of this solution are those of its components (sodium chloride, potassium chloride, and calcium chloride).
The volume and the ionic composition of the extracellular and the intracellular compartments are as follows:
Extracellular fluid: approximately 19 litres
Sodium (mmol/l): | 142 |
Potassium (mmol/l): | 5 |
Calcium (mmol/l): | 2.5 |
Chloride (mmol/l): | 103 |
Intracellular fluid: approximately 23 litres
Sodium (mmol/l): | 15 |
Potassium (mmol/l): | 150 |
Calcium (mmol/l): | 1 |
Chloride (mmol/l): | 1 |
After injection of radiosodium (24 Na), the half-life is 11 to 13 days for 99% of the injected Na and one year for the remaining 1%. The distribution varies according to tissues: it is fast in muscles, liver, kidney, cartilage and skin; it is slow in erythrocytes and neurones; it is very slow in the bone. Sodium is predominantly excreted by the kidney, but there is extensive renal reabsorption. Small amounts of sodium are lost in the faeces and sweat.
Factors influencing potassium transfer between intracellular and extracellular fluid such as acid-base disturbances can distort the relationship between plasma concentrations and total body stores. Potassium is excreted mainly by the kidneys; it is secreted in the distal tubules in exchange of sodium or hydrogen ions. The capacity of the kidneys to conserve potassium is poor and some urinary excretion of potassium continues even when there is severe depletion. Some potassium is excreted in the faeces and small amounts may also be excreted in sweat.
The concentration of calcium in plasma is regulated by parathyroid hormone, calcitonin, and vitamin D. About 47% of calcium in plasma is in the ionised physiologically active form, about 6% is complexed with anions such as phosphate or citrate, and the remainder is bound to proteins, principally albumin. If the plasma-albumin concentration is raised (as in dehydration) or reduced (as is common in malignancy) it will affect the proportion of ionised calcium. Thus, the total plasma-calcium concentration is commonly adjusted for plasma albumin. Excess of calcium is predominantly excreted renally. Unabsorbed calcium is eliminated in the faeces, together with that secreted in the bile and pancreatic juice. Minor amounts are lost in the sweat, skin, hair, and nails. Calcium crosses the placenta and is distributed into breast milk.
Preclinical safety data of Ringer's Injection U.S.P. in animals are not relevant since its constituents are physiological components of animal and human plasma.
Toxic effects are not to be expected under the condition of clinical application.
The safety of potential additives should be considered separately.
The excipients in each 100 ml are:
Water for Injection | Q.S. to 100 ml |
Incompatibility of the medicinal product to be added with the solution in container must be assessed before addition.
Ceftriaxone: See sections 4.3 and 4.4 for more information
In the absence of compatibility studies, this solution must not be mixed with other medicinal products.
The Instructions for Use of the medicinal product to be added must be consulted. Before adding a drug, verify it is soluble and stable in water at the pH of Ringer's Injection U.S.P. (see section 3).
Calcium salts have been reported to be incompatible with a wide range of drugs. Complexes may form resulting in the formation of a precipitate.
As a guidance, the following medications are incompatible with the Ringer's Injection (non-exhaustive listing):
- Amphotericin B
- Cortisone
- Erythromycin lactobionate
- Etamivan
- Ethyl alcohol
- Thiopental sodium
- Disodium edetate
Those additives known to be incompatible should not be used.
§ Keep in a safe place, out of the reach and sight of children.
§ Store below 25° C.
Bottle size: 500 ml × 10 Bottles
Sterile, pyrogen free.
Polyethylene granules:
White colored, round to oblong shaped granules, which are used for the production of containers for intravenous solutions.
Discard after single use.
Discard any unused portion.
Do not reconnect partially used bottle.
Opening
§ If leaks are found, discard solution, as sterility may be impaired
§ Check solution for limpidity and absence of foreign matter. If solution is not clear or contains foreign matter, discard the solution.
Preparation for administration
Use sterile material for preparation and administration.
§ Suspend container from eyelet support.
§ Remove plastic protector from outlet port at bottom of container:
§ Use an aseptic method to set up the infusion.
§ Attach administration set. Refer to directions of the accompanying set for connection, priming of the set and administration of the solution.
Techniques for injection of additive medications
Warning: Additives may be incompatible.
When additive is used, verify isotonicity prior to parenteral administration. Thorough and careful aseptic mixing of any additive is mandatory. Solutions containing additives should be used immediately and not stored.
To add medication before administration
§ Disinfect medication site.
§ Using syringe with 19 to 22 gauge needle, puncture re-sealable medication port and inject.
§ Mix solution and medication thoroughly. For high-density medication such as potassium chloride, tap the ports gently while ports are upright and mix.
Caution: Do not store bottles containing added medications.
To add medication during administration
§ Close clamp on the set
§ Disinfect medication site.
§ Using syringe with 19 to 22 gauge needle, puncture resealable medication port and inject.
§ Remove container from IV pole and/or turn to an upright position.
§ Evacuate both ports by tapping gently while the container is in an upright position.
§ Mix solution and medication thoroughly.
§ Return container to in use position, re-open the clamp and continue administration.
