Comparison of enteral and parenteral methods of urine alkalinization in patients receiving high-dose methotrexate

Rouch, Jamie A; Burton, Bradley; Dabb, Alix; Brown, Vicky; Seung, Amy Hatfield; Kinsman, Katharine; Holdhoff, Matthias

doi:10.1177/1078155215610914

Cited by 17 publications

(26 citation statements)

References 8 publications

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“…We demonstrated in our study no significant difference in MTX clearance rate, which is similar to previous studies using PO sodium bicarbonate 7. There are several limitations to this study.…”

Section: Discussionsupporting

confidence: 90%

“…Roy et al investigated an PO alkalization regimen similar to ours with sodium bicarbonate and PO acetazolamide; however, they used higher doses and more frequent PO sodium bicarbonate and reserved acetazolamide for use as needed when urine pH was <7.5 15Table 6Overview of previously published alternative regimens to intravenous sodium bicarbonate for urine alkalizationAuthorRegimenComparator armOutcomesAdverse eventsShamash et al8Acetazolamide 500 mg IV every 6 hrs for 48 hNo comparatorNo delayed clearanceNo significant AEsRouch et al7Sodium bicarbonate: 650 mg tablet orsodium citrate 500 mg/ citric acid 334 mg/ 5 mL every 6 hrsParenteral sodium bicarbonate (50–150 mEq) physician preferenceNo difference in AKI or hepatic injuryDiarrhea P =0.002Visage et al17Sodium bicarbonate: 1950 mg/m 2 or Sodium citrate-citric acid oral solution: 22.5 mEq/m 2 /dose every 6 hrsNo comparatorDelayed clearance seen in 2% of casesGI side effects reported in 43%Roy et al15Sodium bicarbonate: 3250 mg PO every 12 hrsAcetazolamide 250 mg-500 mg PO or IV every 6 hrs PRN urine pH <7.5+ possible outpatient alkalinizationIntravenous sodium bicarbonate (150 mEq per 1000 mL) AND oral sodium bicarbonate at 3250 PO every 4 hrs PRN for urine pH <7.5No difference in MTX clearanceIncrease in LOS P =0.23No difference in toxicity (AKI, hepatoxicity, myelosuppression)No difference in change in creatinine clearanceAlrabiah et al18Sodium acetate IVParenteral sodium bicarbonateNo difference in LOS, time to pH >8, MTX clearance, or AKINo adverse events identified Abbreviations: MTX, methotrexate; PO, oral; IV, intravenous; LOS, length of stay; PRN, as needed; GI, gastrointestinal. …”

Section: Discussionmentioning

confidence: 99%

“…At the time of the shortage, there were limited published data on the use of PO regimens to achieve urine alkalization in patients receiving HDMTX. Rouch et al detailed the safety and feasibility of utilizing PO sodium bicarbonate tablets and sodium citrate/citric acid suspension but did not define a standard dose 7. Shamash et al utilized an acetazolamide monotherapy regimen; however, there were concerns at our institution that prolonged carbonic anhydrase inhibition may lead to metabolic acidosis, the eventual inability to concentrate bicarbonate ions in the urine, and potentially, AKI.…”

Section: Introductionmentioning

confidence: 99%

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<p>A prospective study on urine alkalization with an oral regimen consisting of sodium bicarbonate and acetazolamide in patients receiving high-dose methotrexate</p>

Reed

Pierce

Sen

et al. 2019

CMAR

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Purpose Intravenous (IV) sodium bicarbonate is typically used in alkalization regimens for the safe use of the chemotherapeutic agent high-dose methotrexate (HDMTX). Urine parameters including urine output and pH are important in order to minimize the risk of kidney injury, which increases adverse effects and hospital length of stay following HDMTX. IV sodium bicarbonate has been on shortage, and there are limited literature describing the safety of alternative regimens. Patients and methods A single institution, prospective analysis of non-Hodgkin’s lymphoma and acute lymphoblastic leukemia patients receiving HDMTX for central nervous system (CNS) prophylaxis or disease. Patients received an oral (PO) regimen of sodium bicarbonate and acetazolamide to achieve a urine pH >7. This cohort was compared to a subsequent IV sodium bicarbonate control cohort. Multiple co-primary safety outcomes assessed the incidences of acute kidney injury and delayed methotrexate clearance as well as change in liver function tests. Secondary outcomes included time to urine pH, time to urine output, and length of stay. Results A total of 126 encounters were studied for the primary safety outcome. There was no difference between AKI incidence in patients receiving the PO alkalization regimen compared to patients receiving IV sodium bicarbonate (14.5% vs 9.3%, respectively, P =0.41). There was no difference in methotrexate clearance between the PO and IV groups (26.5% vs 37.2%, respectively, P =0.21). The use of PO alkalization regimen is estimated to have saved 2002 vials of IV sodium bicarbonate and was approximately US$226 less expensive per encounter. Conclusion This analysis supports the use of PO regimens to achieve urine alkalization necessary for safe administration of HDMTX during periods of IV sodium bicarbonate shortage. Further studies may determine optimal dosing strategies that decrease length of stay and ensure noninferiority of efficacy outcomes with PO regimens for urine alkalization with HDMTX.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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<p>A prospective study on urine alkalization with an oral regimen consisting of sodium bicarbonate and acetazolamide in patients receiving high-dose methotrexate</p>

Reed

Pierce

Sen

et al. 2019

CMAR

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“…Methotrexate excretion can be enhanced by hydration with >3 L/m 2 per day to maximize urine output [ 3 ]. Methotrexate can precipitate in the acidic urine causing crystalluria, hence alkalinizing the urine with oral or parenteral sodium bicarbonate can help prevent this and improve methotrexate excretion [ 18 ]. Another way to enhance elimination is via extracorporeal methods such as hemodialysis, high-flux hemodialysis, plasma exchange, and continuous renal replacement therapy [ 19 ].…”

Section: Discussionmentioning

confidence: 99%

A Rapidly Fatal Case of Low-Dose Methotrexate Toxicity

Shaikh

Sardar

Raj

et al. 2018

Case Reports in Medicine

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An 82-year-old female presented with multiple oral ulcers and malena for 1 week. Her laboratory tests revealed pancytopenia and acute renal failure. She had history of rheumatoid arthritis for which she was taking 7.5 mg methotrexate weekly and stage 4 chronic kidney disease from diabetic nephropathy. During the hospital stay, she developed pneumonia and septic shock requiring norepinephrine and vasopressin. She underwent continuous venovenous hemodiafiltration. Leucovorin, filgrastim, and multiple packed red blood cell and platelet transfusions were given. She remained hypotensive and pancytopenic despite all interventions. She died on day 6 of hospital stay from acute hypoxic respiratory failure due to septic shock.

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“…Одним из маркеров предшествующей нефротоксичности служит снижение клиренса креатинина до начала введения ВДMTX [14]. Ранее считалось, что нормальный уровень креатинина сыворотки и расчетный клиренс креатинина больше 60 мл/мин позволяет обеспечить адекватную элиминацию МТХ, однако на сегодня известно, что токсические эффекты могут развиться даже при адекватной функции почек [25].…”

Section: жизнеугрож ающие ос ложнения при использовании высоких доз мunclassified

Prevention of toxicity in chemotherapy with high doses of methotrexate in children

et al. 2019

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Methotrexate (MTX) is a widely used anti-tumor drug, folic acid antagonists. The effectiveness of high doses (more than 1 g/m2) of MTX in a monotherapy or in a combination with other chemotherapeutic drugs has been proven in a treatment of a large spectrum of oncological diseases in children such as osteosarcoma, tumors of the central nervous system, lymphomas, acute lymphoblastic leukemia. The use of high doses of MTX is often fraughted with development of life-threatening complications such as MTX-induced acute kidney injury, neurotoxicity, myelosuppression. Currently developed recommendations for therapeutic monitoring and supportive care, including hyper-hydration, urine alkalization and leucovorin therapy, allow to reduce toxicity of MTX, but in some patients it is not always possible to prevent the development of complications. Cohort studies in order to identify risk factors for toxicity after high doses of MTX in children with different forms of cancer are limited, as well as comparing various types of supportive care regimens, including, infusion therapy. Studying of development mechanisms of MTX toxicity depending on background conditions will allow to improve existing recommendations and develop new and most effective standards of supportive therapy with respect to the individual specifics of patients.

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Comparison of enteral and parenteral methods of urine alkalinization in patients receiving high-dose methotrexate

Cited by 17 publications

References 8 publications

<p>A prospective study on urine alkalization with an oral regimen consisting of sodium bicarbonate and acetazolamide in patients receiving high-dose methotrexate</p>

<p>A prospective study on urine alkalization with an oral regimen consisting of sodium bicarbonate and acetazolamide in patients receiving high-dose methotrexate</p>

A Rapidly Fatal Case of Low-Dose Methotrexate Toxicity

Prevention of toxicity in chemotherapy with high doses of methotrexate in children

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