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Query: UMLS:C0162316 (
iron deficiency anemia
)
3,806
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
This case series describes the cases of three adolescent patients with established
inflammatory bowel disease
(
IBD
) who experienced significant hypophosphataemia following intravenous infusion of ferric carboxymaltose as treatment for
iron deficiency anaemia
. Hypophosphataemia may cause a diverse range of symptoms and may be difficult to diagnose clinically due to their non-specific nature. Checking a baseline phosphate (PO
4
) prior to intravenous iron infusion may identify patients at higher risk for significant hypophosphataemia and perhaps allow the selection of an alternative iron preparation. The routine monitoring of PO
4
levels postinfusion presents a greater challenge; with cases of asymptomatic hypophosphataemia likely to be uncovered, as in case 3. Clinicians, patients and families should be aware of the symptoms of hypophosphataemia, and symptomatic patients should have bloods checked to allow prompt identification and correction of abnormalities where required. Review of guidelines surrounding intravenous iron infusion and management of hypophosphataemia in paediatric patients is now required.
...
PMID:Severe hypophosphataemia following ferric carboxymaltose infusion in paediatric patients with inflammatory bowel disease. 3258 74
Objective:
To review the pharmacology, efficacy, and safety of ferric maltol (FM), an oral iron formulation, for
iron deficiency anemia
(
IDA
).
Data Sources:
A MEDLINE/PubMed and EMBASE (January 1, 1985, to June 19, 2020) literature search was performed using the terms
ferric maltol, accrufer, feraccru, iron maltol, ferric trimaltol, iron deficiency,
iron deficiency anemia
,
inflammatory bowel disease
, and
chronic kidney disease
. Additional data sources included prescribing information, abstracts, and the National Institutes of Health Clinical Trials Registry.
Study Selection/Data Extraction:
English language literature evaluating FM pharmacology, pharmacokinetics, efficacy, or safety in the treatment of
IDA
were reviewed.
Data Synthesis:
FM is a ferric, non-salt-based oral iron formulation demonstrating improved tolerance in patients with previous intolerance to other iron formulations. Phase 3 trials demonstrated significant improvements in anemia and serum iron parameters in patients with
inflammatory bowel disease
(
IBD
) and chronic kidney disease (CKD). Common adverse effects were gastrointestinal intolerance.
Relevance to Patient Care and Clinical Practice:
FM is an effective and well-tolerated alternative to oral iron salts for patients with
IBD
or CKD and
IDA
. Emerging data suggest that FM is noninferior to intravenous (IV) ferric carboxymaltose in patients with
IBD
and
IDA
. Prior to selecting FM over IV iron products, consideration should be given to time to normalization of Hb, ease of administration, cost, and tolerability.
Conclusion:
FM is a relatively safe, effective oral iron therapy that may be better tolerated than other oral iron formulations. FM may be an effective alternative to IV iron in patients with
IBD
.
...
PMID:Ferric Maltol: A New Oral Iron Formulation for the Treatment of Iron Deficiency in Adults. 3263 48
We report a 45-year-old healthy Chinese woman who presented with chronic diarrhea and
iron deficiency anemia
, with colonoscopy showing multiple ulcers from cecum to sigmoid on a background of dark-purple mucosa. She was initially suspected to be suffering from
inflammatory bowel disease
, but the peculiar colonic biopsy findings and computed tomography (CT) imaging features, together with her habit of using Chinese herbal supplements, supported the rare diagnosis of idiopathic mesenteric phlebosclerosis.
...
PMID:Idiopathic mesenteric phlebosclerosis: A rare cause of chronic diarrhea. 3278 70
We report a case of an African American woman who presented with fatigue, generalized weakness, and hypophosphatemia in the setting of a recent hospitalization for severe, symptomatic
iron deficiency anemia
requiring ferric carboxymaltose infusions. Parental iron is indicated in numerous clinical settings including chronic kidney disease,
inflammatory bowel disease
, and
iron deficiency anemia
. Ferric carboxymaltose is one of the most common forms of parental iron infusions used due to administration procedure and minimal reported side effects. The most common side effect reported is a transient decrease in serum phosphate. This case highlights the necessity of monitoring serum phosphate in the setting of parental iron infusions, especially ferric carboxymaltose, and when severe hypophosphatemia occurs management includes intravenous phosphorous and calcitriol.
...
PMID:A rare case of parental iron-induced persistent hypophosphatemia. 3285 57
Iron deficiency anemia
is the most common type of anemia, and it occurs when the human body does not have enough of the mineral iron (https://www.healthline.com/health/iron-deficiency-anemia#diagnosis).
Iron deficiency anemia
is caused by blood loss, insufficient dietary intake, or poor absorption of iron from food. Sources of blood loss can include heavy periods, childbirth, uterine fibroids, stomach ulcers, colon cancer, and urinary tract bleeding (https://www.nhlbi.nih.gov/health-topics/iron-deficiency-anemia). Poor absorption of iron from food may occur as a result of an intestinal disorder such as
inflammatory bowel disease
or celiac disease, or surgery such as a gastric bypass (https://www.who.int/nutrition/topics/ida/en/). Little is known about the association between
iron deficiency anemia
and lymphocytopenia. Here, we report on a 17-year-old female who presented with
iron deficiency anemia
and was found to have lymphopenia. She recovered after having received intravenous iron therapy.
...
PMID:Iron Deficiency Anemia-Induced Lymphocytopenia in a Young Female. 3288 20
Anemia is the most common extraintestinal systemic complication of
inflammatory bowel disease
.
Iron deficiency anemia
and anemia of chronic disease are among the most frequent types. Intestinal iron absorption is controlled by the activity of ferroportin. Cells with high expression of ferroportin include enterocytes, and also macrophages and hepatocytes. Iron homeostasis is controlled by the hepcidin-ferroportin axis. Hepcidin is a central regulator of iron metabolism and can also serve as a marker of systemic inflammation. During systemic inflammatory response, the synthesis of hepcidin increases, and hepcidin binds to ferroportin and inhibits its activity. Thus, iron is not absorbed from the bowel into the circulation and also remains sequestered in macrophages. Conversely, hepcidin synthesis is suppressed during conditions requiring increased iron intake for enhanced erythropoiesis, such as
iron deficiency anemia
or hypoxia. Here, ferroportin is not blocked, and iron is actively absorbed into the bloodstream and also released from the stores. Production of hepcidin is influenced by the status of total body iron stores, systemic inflammatory activity and erythropoietic activity. Oral iron therapy is limited in inflammatory bowel diseases due to ongoing gastrointestinal inflammation. It is less effective and may worsen the underlying disease. Therefore, the choice between oral and parenteral iron therapy must be made with caution. Oral iron would be ineffective at high hepcidin levels due to concurrent ferroportin blockage. Contrarily, low levels of hepcidin indicate that oral iron therapy should be successful. An understanding of hepcidin can help in understanding the body's reaction to iron depletion during the inflammatory process.
...
PMID:Importance of Hepcidin in the Etiopathogenesis of Anemia in Inflammatory Bowel Disease. 3306 92
The most common complication seen in
inflammatory bowel disease
(
IBD
) patients is
iron deficiency anaemia
(
IDA
). Symptoms such as chronic fatigue can be as debilitating to
IBD
patients as pathological symptoms of abdominal pain and diarrhoea. Recognising and correcting anaemia may be as important as managing
IBD
symptoms and improving overall quality of life. Thus, iron replacement should be commenced the moment
IDA
is identified. Although intravenous iron is now considered standard treatment for
IBD
patients in Europe, oral iron still appears to be the preferred option. Advantages of oral iron include greater availability, lower costs and ease of applicability. However, its multitude of side effects, impact on the microbiome and further exacerbating
IBD
activity can have consequences on patient compliance. The newer oral iron formulations show promising safety and efficacy data with a good side effect profile. Intravenous iron formulations bypass the gastrointestinal tract absorption thereby leading to less side effects. Multiple studies have shown its superiority compared to oral formulations although its risk for hypersensitivity reactions continue to lead to clinician hesitancy in prescribing this formulation. This article provides an updated review on diagnosis and management of
IDA
in
IBD
patients, discussing the newer oral and intravenous formulations.
...
PMID:Iron Therapy in Inflammatory Bowel Disease. 3319 76
Up to 30-70% of patients may experience mild and moderate side effects during iron therapy and this is often associated with a poor adherence to therapy. Anemia is frequent in patients with active
inflammatory bowel disease
(
IBD
), due to both iron deficiency and chronic inflammation, therefore iron supplementation is frequently needed. Considering that gastrointestinal disorders are the most common side effects with oral iron, in
IBD
patients intravenous administration must be preferred. Although intravenous iron supplementation remains the most effective therapy of
IBD
-associated
iron deficiency anemia
, the perception of risk related to intravenous administration by clinicians could limit this successful strategy. In this narrative review we provide an up-to-date on the safety of the different iron formulations for intravenous administration, by reporting the most recent studies in
IBD
patients.
...
PMID:Safety profile of intravenous iron in inflammatory bowel disease: an up-to-date overview. 3326 72
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