High Dose Erythropoietin versus desidustat for treatment of anemia in patients of chronic kidney disease having inadequate response to weight based erythropoietin dose: A prospective randomised control study

Start Date22 Jan 2024

Sponsor / Collaborator-

IRCT20230901059316N1

/ RecruitingPhase 3IIT

Investigating the neuroprotective effect of erythropoietin in patients with severe traumatic brain injury

Start Date21 Jan 2024

Sponsor / Collaborator

Mashhad University of Medical Sciences

100 Clinical Results associated with Erythropoietin(Xiamen Amoytop Biotech Co. Ltd.)

100 Translational Medicine associated with Erythropoietin(Xiamen Amoytop Biotech Co. Ltd.)

100 Patents (Medical) associated with Erythropoietin(Xiamen Amoytop Biotech Co. Ltd.)

1,112

Literatures (Medical) associated with Erythropoietin(Xiamen Amoytop Biotech Co. Ltd.)

01 May 2025·Journal of clinical orthopaedics and trauma

Conservative and newer drug treatment for degenerative cervical myelopathy

Article

Author: Ede, Osita ; Cheung, Jason Pui Yin

Degenerative cervical myelopathy (DCM) is the most common cause of non-traumatic spinal cord dysfunction in adults worldwide. Conservative treatments, such as physical therapy, activity modification, cervical traction, and the use of cervical collars, have been employed primarily for symptomatic relief in mild cases or for patients deemed unfit for surgery. Advances in our understanding of the molecular pathways involved in neuroinflammation and neuronal injury in DCM have spurred the development of newer pharmacological treatments aimed at neuroprotection and inflammation control. We found limited evidence that conservative treatment enhances functional recovery in patients with DCM. Patients with mild DCM who opt for conservative therapy should be aware of likely neurological deterioration and higher spinal cord injury risk following neck trauma. Nonoperative management could benefit patients with mild DCM who presented early (at least less than a year), have soft disc herniation as the cause of the myelopathy, have one level of myelopathic compression, and whose MRI does not show circumferential compression of the spinal cord. Riluzole did not replicate its promising animal results in human trials, using the modified Japanese Orthopaedic Association (mJOA) score as an outcome measure. Cerebrolysin is promising but needs more RCTs to define its role in the management algorithm. Limaprost Alfadex provided inconclusive evidence, however, is in an ongoing phase III trial. Erythropoietin showed benefit in animal and human trials but concerns over side effects may limit use. G-CSF demonstrated evidence of preserved neurological function in mice but needs human studies. Steroids did not show benefit and are likely deleterious to tissue healing and can increase infection risk. Anti-Fas ligand antibody has not been studied in humans but demonstrated benefit in animal models. Research should focus on large-scale RCTs for these drugs with careful attention to long-term effects, side effects, and finding the most effective doses.

01 Mar 2025·JOURNAL OF MUSCLE RESEARCH AND CELL MOTILITY

Enduring effects of acute prenatal ischemia in rat soleus muscle, and protective role of erythropoietin

Article

Author: Dereumetz, Julie ; Bastide, Bruno ; Canu, Marie-Hélène ; Sancerni, Tiphaine ; Coq, Jacques-Olivier ; Cochon, Laetitia ; Montel, Valérie

Motor disorders are considered to originate mainly from brain lesions. Placental dysfunction or maternal exposure to a persistently hypoxic environment is a major cause of further motor disorders such as cerebral palsy. Our main goal was to determine the long-term effects of mild intrauterine acute ischemic stress on rat soleus myofibres and whether erythropoietin treatment could prevent these changes. Rat embryos were subjected to ischemic stress at embryonic day E17. They then received an intraperitoneal erythropoietin injection at postnatal days 1-5. Soleus muscles were collected at postnatal day 28. Prenatal ischemic stress durably affected muscle structure, as indicated by the greater fiber cross-sectional area (+ 18%) and the greater number of mature vessels (i.e. vessels with mature endothelial cells) per myofibres (+ 43%), and muscle biochemistry, as shown by changes in signaling pathways involved in protein synthesis/degradation balance (-81% for 4EBP1; -58% for AKT) and Hif1α expression levels (+ 95%). Erythropoietin injection in ischemic pups had a weak protective effect: it increased muscle mass (+ 25% with respect to ischemic pups) and partially prevented the increase in muscle degradation pathways and mature vascularization, whereas it exacerbated the decrease in synthesis pathways. Hence, erythropoietin treatment after acute ischemic stress contributes to muscle adaptation to ischemic conditions.

28 Feb 2025·Giornale italiano di nefrologia : organo ufficiale della Societa italiana di nefrologia

Balancing Efficacy, Health Status, and Cost-Effectiveness: A Comparative Study of Desidustat and Erythropoietin in Chronic Kidney Disease Patients on Hemodialysis.

Article

Author: Yarramachu, Dharanidhar Reddy ; Elayaperumal, Indhumathi ; Singh, K Sai Sindhu ; Manoj, Kumar K ; Lakshmi Aishwarya, Pavuluri

Background. Anemia is a common problem that greatly affects the quality of life and prognosis of those with CKD (chronic kidney disease). The conventional course of treatment has traditionally used ESAs (erythropoiesis-stimulating agents) such as erythropoietin; however, more recent medications, such as Desidustat, a hypoxia-inducible factor prolyl hydroxylase inhibitor (HIF-PHI), may be more advantageous in terms of both efficacy and cost. In this study, CKD patients receiving hemodialysis are compared for efficacy, safety, and cost-effectiveness between Desidustat and erythropoietin treatment. Methods. This prospective, single-center, open-label study with parallel groups was carried out at Saveetha Institute of Medical Sciences in Chennai. A total of 60 patients with CKD on maintenance hemodialysis were randomized to receive either Desidustat (100 mg orally, 3 times a week) or Erythropoietin (subcutaneous injections) for 12 weeks. At baseline, four weeks, eight weeks, and 12 weeks, hemoglobin levels, biomarkers (TSAT, ferritin, and hepcidin), and status of physical and mental health had been noted. The key finding was the proportion of hemoglobin responders (defined as a rise from baseline of ≥1g/dL). Secondary outcomes included predictors of hemoglobin response, adverse effects, and cost-effectiveness. Results. The proportion of hemoglobin responders was 83.33% in the Desidustat compared to 73.33% in the Erythropoietin group (p = 0.530), indicating no significant difference in efficacy. Hemoglobin levels increased gradually in both groups over 12 weeks. Higher serum albumin (OR = 3.32, 95% CI: 1.54-7.16, p = 0.008) and lower iPTH levels (OR = 0.98, 95% CI: 0.97-0.99, p = 0.004) have been important indicators of hemoglobin response. Hepcidin levels decreased significantly in the Desidustat group in contrast to Erythropoietin (p = 0.038), suggesting improved iron metabolism with Desidustat. No significant differences were noted in TSAT or ferritin levels. Adverse effects were comparable between the groups, with similar hospitalization and infection rates. Desidustat demonstrated better cost-effectiveness, with a lower monthly cost compared to Erythropoietin. Conclusions. When treating anemia in individuals with CKD receiving hemodialysis, Desidustat is a safe and efficient substitute for erythropoietin, with the added advantage of cost-effectiveness. Serum albumin and iPTH were significant predictors of hemoglobin response. To validate these results larger multicentric studies are necessary.

News (Medical) associated with Erythropoietin(Xiamen Amoytop Biotech Co. Ltd.)

12 Mar 2025

·pipelinereview.com

Geron Announces European Commission Approval of RYTELO® (imetelstat), a First-in-Class Telomerase Inhibitor, for the Treatment of Adults With Transfusion-Dependent Anemia Due to Lower-Risk MDS

FOSTER CITY, CA, USA I March 11, 2025 I Geron Corporation (Nasdaq: GERN), a commercial-stage biopharmaceutical company aiming to change lives by changing the course of blood cancer, today announced that the European Commission (EC) has granted marketing authorization for RYTELO® (imetelstat) as a monotherapy for the treatment of adult patients with transfusion-dependent (TD) anemia due to very low, low or intermediate risk myelodysplastic syndromes (lower-risk MDS or LR-MDS) without an isolated deletion 5q cytogenetic (non-del 5q) abnormality and who had an unsatisfactory response to or are ineligible for erythropoietin-based therapy (ESAs). Lower-risk MDS is a progressive blood cancer with high unmet need, where many patients with anemia become dependent on red blood cell transfusions, which can be associated with clinical consequences and decreased quality of life. “As the first and only treatment of its kind, RYTELO represents an important new option – significantly reducing the need for red blood cell transfusions for people living with LR-MDS who are battling debilitating symptoms like anemia and fatigue,” said Joseph Eid, M.D., Geron’s Executive Vice President, Research and Development. “This approval from the European Commission, just nine months following approval in the U.S., underscores the positive benefit for these patients demonstrated in our clinical trials and we look forward to making this innovative therapy accessible to eligible patients in Europe.” “I am thrilled that the European Commission has approved RYTELO in LR-MDS. The long-term and durable responses observed in the Phase 3 IMerge study reinforce the practice-changing potential of telomerase inhibition as a clinically meaningful and differentiated option for the treatment of lower-risk MDS,” said Uwe Platzbecker, M.D., Chief Medical Officer at the University Hospital Carl Gustav Carus Dresden in Germany, who was an IMerge investigator and a co-lead author of the Phase 3 results published in The Lancet . “Physicians and patients in Europe are now one step closer to accessing a novel treatment that, in addition to having a generally manageable safety profile, has the potential to provide extended and continuous red blood cell transfusion independence.” The marketing authorization of RYTELO approved by the EC is supported by data from the IMerge Phase 3 clinical trial, which demonstrated the significant clinical benefit of RYTELO in patients with transfusion-dependent anemia due to LR-MDS, reducing the need for red blood cell transfusions in the first 24 weeks of treatment compared to placebo, as observed in the double-blind controlled study. The safety profile of RYTELO was well-characterized with generally manageable and short-lived thrombocytopenia and neutropenia, which are familiar side effects for hematologists who are experienced with managing cytopenias. The most commonly reported adverse reactions ≥ Grade 3 were neutropenia (69%), thrombocytopenia (63%), which lasted a median duration of less than two weeks, and in more than 80% of patients were resolved to Grade < 2 in under four weeks. RYTELO is the first and only telomerase inhibitor approved by the EC, and the marketing authorization applies to all 27 European Union member states, and Iceland, Norway and Liechtenstein. Geron is preparing to commercialize RYTELO in select EU countries beginning in 2026, pending country-by-country reimbursement. Additionally, Geron is exploring opportunities to make RYTELO available to eligible patients through Expanded Access Programs (EAP), including Named Patient Programs (NPP), which are designed to support access for individual patients on a case-by-case basis. In connection with the approval, the EMA’s Committee of Orphan Medicinal Products (COMP) reviewed and issued a positive opinion to maintain RYTELO’s orphan drug designation in the EU for MDS, which is expected to provide market exclusivity for ten years after approval, subject to maintaining orphan designation. Patent exclusivity in the EU for LR-MDS is anticipated into 2038, subject to approval of patent term extension by the European Patent Office. About Lower-Risk Myelodysplastic Syndromes (LR-MDS) Lower-risk myelodysplastic syndromes (LR-MDS) is a blood cancer that often progresses to require increasingly intensified management of key symptoms such as anemia and resulting fatigue 1 . These symptomatic LR-MDS patients frequently become red blood cell transfusion dependent, which has been shown to be associated with short- and long-term clinical consequences that reduce quality of life and shorten survival 2,3 . There is a high unmet need for many LR-MDS patients, particularly those with characteristics having poorer prognosis. Current treatment options for those failing ESA are limited to select sub-populations and there is an unmet need for treatments that can provide extended and continuous red blood cell transfusion independence. About RYTELO® (imetelstat) RYTELO is an oligonucleotide telomerase inhibitor approved in the U.S. for the treatment of adult patients with low-to-intermediate-1 risk myelodysplastic syndromes (LR-MDS) with transfusion-dependent anemia requiring four or more red blood cell units over eight weeks who have not responded to or have lost response to or are ineligible for erythropoiesis-stimulating agents (ESAs). It is indicated to be administered as an intravenous infusion over two hours every four weeks. In addition, RYTELO is approved in the European Union as a monotherapy for the treatment of adult patients with transfusion-dependent anemia due to very low, low or intermediate risk myelodysplastic syndromes without an isolated deletion 5q cytogenetic (non-del 5q) abnormality and who had an unsatisfactory response to or are ineligible for erythropoietin-based therapy. RYTELO is a first-in-class treatment that works by inhibiting telomerase enzymatic activity. Telomeres are protective caps at the end of chromosomes that naturally shorten each time a cell divides. In LR-MDS, abnormal bone marrow cells often express the enzyme telomerase, which rebuilds those telomeres, allowing for uncontrolled cell division. Developed and exclusively owned by Geron, RYTELO is the first and only telomerase inhibitor approved by the U.S. Food and Drug Administration and the European Commission. Please see RYTELO (imetelstat) full Prescribing Information, available at https://pi.geron.com/products/US/pi/rytelo_pi.pdf . The Summary of Product Characteristics (SmPC) for RYTELO in the EU is available at https://pi.geron.com/products/rytelo/eu/rytelo_smpc_eu.pdf About Geron Geron is a commercial-stage biopharmaceutical company aiming to change lives by changing the course of blood cancer. Our first-in-class telomerase inhibitor RYTELO™ (imetelstat) is approved in the United States and the European Union for the treatment of certain adult patients with lower-risk myelodysplastic syndromes (LR-MDS) with transfusion-dependent anemia. We are also conducting a pivotal Phase 3 clinical trial of imetelstat in JAK-inhibitor relapsed/refractory myelofibrosis (R/R MF), as well as studies in other hematologic malignancies. Inhibiting telomerase activity, which is increased in malignant stem and progenitor cells in the bone marrow, aims to potentially reduce proliferation and induce death of malignant cells. To learn more, visit www.geron.com or follow us on LinkedIn . 1 Lewis R, Bewersdorf JP, Zeidan AM. Clinical Management of Anemia in Patients with Myelodysplastic Syndromes: An Update on Emerging Therapeutic Options. Cancer Manag Res. 2021 Jan 25;13:645-657. doi: 10.2147/CMAR.S240600. PMID: 33531837; PMCID: PMC7846829. 2 Cogle CR, Reddy SR, Chang E, et al. Early treatment initiation in lower-risk myelodysplastic syndromes produces an earlier and higher rate of transfusion independence. Leuk Res. 2017;60:123-128. 3 Balducci, L. (2006), Transfusion independence in patients with myelodysplastic syndromes. Cancer, 106: 2087-2094. https://doi.org/10.1002/cncr.21860 SOURCE: Geron

Phase 3Drug ApprovalClinical ResultOrphan Drug

100 Deals associated with Erythropoietin(Xiamen Amoytop Biotech Co. Ltd.)

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Indication	Highest Phase	Country/Location	Organization	Date
Anemia in chronic kidney disease	Phase 2	China	Xiamen Amoytop Biotech Co. Ltd.	12 Mar 2021
Anemia of renal disease	Phase 2	China	Xiamen Amoytop Biotech Co. Ltd.	12 Mar 2021
Growth hormone deficiency	Phase 1	China	Xiamen Amoytop Biotech Co. Ltd.	09 Nov 2012
Idiopathic short stature	Phase 1	China	Xiamen Amoytop Biotech Co. Ltd.	09 Nov 2012
Anemia	Phase 1	-	BioGeneric Pharma SAE	-

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


ARVO2019	Phase 2	Optic Nerve Diseases	34	Erythropoietin	wjoogbgksy(spyqlnbkap) = cnncrmjvly iwvifimywj (mdoxdsaeyl ) View more	-	01 Jul 2019
				Placebo	wjoogbgksy(spyqlnbkap) = sglxxuzgps iwvifimywj (mdoxdsaeyl )
CNS2016	Not Applicable	Hypoxia-Ischemia, Brain	-	Erythropoietin 1000 U/kg IV	dkmhitfbjo(exojbjmbcb) = fatqoimjho bugcqtntsu (fbedyyvwiz, 73.8)	Positive	14 Oct 2016
				Placebo	dkmhitfbjo(exojbjmbcb) = vtrbywdrhf bugcqtntsu (fbedyyvwiz, 107.1)
ESC2016	Not Applicable	Hypovolemia	-	PBS pre-treated young rats	cgejagtoue(otlgfgepnf) = zuakqbfalg uwvtzeyido (yvkhuxtiik )	-	28 Aug 2016
				EPO pre-treated young rats	cgejagtoue(otlgfgepnf) = felagbzmqq uwvtzeyido (yvkhuxtiik )
CNS2015	Phase 2	Hypoxia-Ischemia, Brain	50	Erythropoietin	eqgaudkgvh(tqkxcrpbnu) = bjylmwvbyf nyerwfqkdl (nymmsiendi, 0 - 14)	Positive	25 Sep 2015
Off-label study (ARVO2014)	Not Applicable	Age Related Macular Degeneration	32	Procrit 5U	egizuewfaw(fpmdkibnpy) = lntgleaxbr npjtooscwr (agsobesybl ) View more	Positive	01 Apr 2014
AAO2013	Not Applicable	Optic Nerve Diseases	-	Intravenous recombinant erythropoietin 20,000 units	qaurwrqqjn(mmdqixexpq) = ndddmjjjou tdagqahtej (rqnssrdwwp )	Positive	18 Nov 2013
ARVO2012	Not Applicable	Optic Neuritis	-	Erythropoietin (rAAV2/8.CMV.EpoR76E vector)	betjsxdaoa(gabrkgibya) = higher in EPO treated mice as compared to control EAE mice rymwxmwkgk (mvmuasymju ) View more	-	01 Mar 2012
ARVO2011	Not Applicable	Optic Nerve Injuries	-	rAAV.Epo	qyasytxnvr(guyilperpf) = vhkgkviltx xcqymgvnwl (umjqxtizqo ) View more	Positive	01 Apr 2011
				Erythropoietin (rAAV.EpoR76E)	qyasytxnvr(guyilperpf) = wbnwqaxpfw xcqymgvnwl (umjqxtizqo ) View more
ARVO2010	Not Applicable	-	-	Erythropoietin	onployepzr(tlxieulbat) = wzmjrzwzxo wmciegfzzi (bbvazwggpj )	-	01 Apr 2010
ARVO2008	Not Applicable	Diabetic Retinopathy	60	Erythropoietin (Diabetics with retinopathy)	krixpjnruj(dvjeqbdsuo) = ciirvasxdr fhbnistslk (cluzqdaklk )	-	01 May 2008
				Erythropoietin (Diabetics without retinopathy)	krixpjnruj(dvjeqbdsuo) = ciybqyobpq fhbnistslk (cluzqdaklk )

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