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pharma · Nasopharyngeal Carcinoma · Hepatocellular Carcinoma

Chinese Academy of

Chinese Academy of is a pharma organization headquartered in TAIZHOU, CN. Primary therapeutic focus areas include Nasopharyngeal Carcinoma, Hepatocellular Carcinoma, COVID-19, Breast Cancer, Coronary Artery Disease. Nova

China, TAIZHOU, CN HQ
170 Employees
NMPA registrant Type
Company details
Status
Public
HQ
China, TAIZHOU, CN
Employees
170
Programs
1328
Drugs
711
Patents
335
Clinical program

Oral supplementation of vitamin D

Unknown · other · Obesity

Oral supplementation of vitamin D (internal code VD50kIU2011) is a completed clinical program sponsored by Xiyuan Hospital of China Academy of Chinese Medical Sciences investigating the use of vitamin D supplementation for obesity management. The program enrolled patients in a clinical trial (NCT01781169) that conclude

Internal code VD50kIU2011

At a glance

Sponsor
Xiyuan Hospital of China Academy of Chinese Medical Sciences
Phase
Unknown
Modality
other
Indication
Obesity
Status
completed
Trials
1

Executive summary

Oral supplementation of vitamin D (internal code VD50kIU2011) is a completed clinical program sponsored by Xiyuan Hospital of China Academy of Chinese Medical Sciences investigating the use of vitamin D supplementation for obesity management. The program enrolled patients in a clinical trial (NCT01781169) that concluded by October 2013. The program evaluates vitamin D's potential metabolic and endocrine effects on weight management, though the specific mechanism of action in obesity remains not yet disclosed. The trial involved oral vitamin D administration, with ergocalciferol (vitamin D2) identified as a key investigational component. Ergocalciferol is an FDA-approved vitamin D receptor agonist with established regulatory status in the United States across multiple generic manufacturers. The program represents an early-stage exploration of micronutrient supplementation as an adjunctive obesity intervention, distinct from contemporary pharmacological weight-loss agents. Development status is completed, with the latest documented milestone occurring on 30 October 2013. No subsequent milestones, regulatory filings, or commercial development plans have been disclosed. The program does not appear to have progressed to formal regulatory submission or approval pathways.

Analyst view

Why this program matters

Obesity remains a significant global public health challenge with limited pharmacological treatment options, particularly in 2011–2013 when this trial was conducted. Vitamin D deficiency has been epidemiologically associated with obesity and metabolic dysfunction in observational studies, creating a rationale for investigating supplementation as a potential intervention. The mechanistic hypothesis—that vitamin D repletion may improve metabolic parameters and support weight loss—addresses an unmet need for safe, accessible, and low-cost obesity treatments, especially in populations with concurrent vitamin D insufficiency. This approach differs fundamentally from contemporary obesity pharmacotherapy (GLP-1 receptor agonists, lipase inhibitors) by targeting a micronutrient deficiency rather than appetite or energy expenditure pathways. The competitive landscape for obesity treatment has evolved substantially since 2013, with newer agents demonstrating superior efficacy. However, vitamin D supplementation remains relevant for specific patient populations with documented deficiency and metabolic dysfunction. The program's completion without apparent regulatory advancement suggests either negative or inconclusive efficacy findings, or a strategic decision to deprioritize micronutrient-based obesity interventions in favor of pharmacological approaches. Market relevance is limited by the availability of over-the-counter vitamin D products and the lack of proprietary formulation or novel mechanism differentiation.

Drug intelligence

Drug Class: Vitamin D supplementation (micronutrient/dietary supplement)

Modality: Other (dietary supplement/micronutrient)

Active Ingredients: Ergocalciferol (vitamin D2) and vitamin (unspecified formulation)

Mechanism of Action: Ergocalciferol functions as a vitamin D receptor agonist, activating the vitamin D3 receptor to modulate calcium homeostasis, immune function, and metabolic pathways implicated in obesity and glucose metabolism.

Route of Administration: Oral

Target: Vitamin D3 receptor

Regulatory Status: Ergocalciferol is FDA-approved as a prescription and over-the-counter product with multiple generic manufacturers (ANDA040833, ANDA040865, and others). No novel formulation or indication-specific approval was sought or obtained for this obesity program.

Related Therapies: Vitamin D supplementation is available globally as a dietary supplement; prescription ergocalciferol is indicated for vitamin D deficiency and hypoparathyroidism, not obesity.

Patent Status: Not yet disclosed; ergocalciferol is off-patent.

Disease intelligence

obesity disorder

Also known as: obesity, obesity disease

Overview

A disorder involving an excessive amount of body fat.

Treatment landscape

ClinicalTrials.gov lists 50 registered studies for Obesity (Disorder) (AACT aggregate).

Phase breakdown: NA (46), PHASE4 (3), PHASE3 (1)

Common investigational therapies:

  • Tirzepatide
  • Placebo
  • Semaglutide Pen Injector
  • Semaglutide
  • Gradual dose reduction of semaglutide
  • Abrupt cessation of semaglutide
  • GLP-1 Receptor Agonists
  • GLP-1 Therapy
  • Semaglutide (SEMA)
  • Metoclopramide

Disease data sourced from MONDO Disease Ontology (MONDO:0011122), Orphanet — obesity disorder, NCT03412149, NCT06787001, NCT06852391, NCT06881485, NCT06911918, AACT (ClinicalTrials.gov aggregate), ClinicalTrials.gov, Open Targets Platform (CC BY 4.0).

Clinical development timeline

  1. Completed2013-10-30

    Trial completion

    Clinical trial NCT01781169 completed; latest documented milestone for the VD50kIU2011 program.

Competitive landscape

The competitive landscape for obesity treatment has shifted substantially since this vitamin D supplementation trial concluded in 2013. Contemporary competitors identified in the facts include semaglutide (Disc Medicine), tirzepatide (Mounjaro, The George Institute), and naltrexone/bupropion (Mysimba, Disc Medicine)—all approved pharmacological agents with demonstrated efficacy in weight reduction. Simvastatin (Hospital Authority, Hong Kong) and pioglitazone (Takeda) represent older metabolic agents with secondary weight effects. Candesartan/hydrochlorothiazide (Takeda) and esomeprazole (Fondazione Telethon) are not primary obesity treatments. The vitamin D supplementation approach differs fundamentally: it targets micronutrient repletion rather than appetite suppression or metabolic enhancement. Unlike GLP-1 agonists or dual GIP/GLP-1 agonists, vitamin D supplementation is non-proprietary, widely available over-the-counter, and lacks the clinical efficacy data supporting contemporary agents. The program's completion without apparent regulatory advancement or commercial development suggests that vitamin D supplementation did not demonstrate sufficient efficacy to compete with emerging pharmacological options. Competitive positioning is further weakened by the lack of novel formulation, patent protection, or differentiated mechanism in obesity management.

TherapyCompanyMechanismStatus
SimvastatinHospital Authority, Hong Kongsmall_moleculeapproved
PioglitazoneTakedasmall_moleculeapproved
Semaglutide B 3.0 mg/ml PDS290Disc Medicinesmall_moleculeapproved
Mounjaro solution for injection in pre-filled... for ObesityThe George Institutesmall_moleculeapproved
ESOMEPRAZOLE, ESOMEPRAZOLEFondazione Telethon ETSsmall_moleculeapproved
Candesartan and HydrochlorothiazideTakedasmall_moleculeapproved
NN9838-4968NovoThirteensmall_moleculeapproved
Intravenous IbuprofenCUMBERLAND PHARMACEUTICALS INCsmall_moleculeapproved
NN9536-7752NovoThirteensmall_moleculeapproved
ANGELOThe George Institutesmall_moleculeapproved
Mysimba 8 mg/90 mg prolonged-release tabletsDisc Medicinesmall_moleculeapproved
RIMEGEPANT , CapsaicinDisc Medicinesmall_moleculeapproved
SIBUTRAMINEMonoamine transporter inhibitorApproved
SETMELANOTIDE ACETATEMelanocortin receptor 4 agonistApproved
SETMELANOTIDEMelanocortin receptor 4 agonistApproved
RIMONABANTCannabinoid CB1 receptor antagonistApproved
PHENTERMINE HYDROCHLORIDENorepinephrine transporter releasing agentApproved
PHENTERMINENorepinephrine transporter releasing agentApproved
PHENDIMETRAZINE TARTRATENorepinephrine transporter inhibitorApproved
ORLISTATPancreatic lipase inhibitorApproved

Additional associated therapies sourced from Open Targets Platform (CC0), linked to NovaPharmaNews drug profiles where matched.

Regulatory intelligence

United States (FDA): Ergocalciferol (vitamin D2) is approved as a prescription and over-the-counter product under multiple ANDA applications (ANDA040833, ANDA040865, ANDA080704, ANDA080747, ANDA080825, ANDA080884, ANDA080951, ANDA080956, ANDA083102, ANDA084053, ANDA090455, ANDA091004, ANDA204276) and NDA003444. Approved indications include vitamin D deficiency and hypoparathyroidism, not obesity. No FDA approval, IND, or NDA submission for obesity indication has been disclosed.

China (NMPA): Vitamin (unspecified) is listed as undergoing clinical trials in China (NCT01317849, NCT02407899, NCT02799134). The VD50kIU2011 program trial (NCT01781169) completed in 2013; regulatory status post-completion is not yet disclosed.

European Medicines Agency (EMA): Not yet disclosed.

Japan (PMDA): Not yet disclosed.

Program Status: The obesity indication for vitamin D supplementation has not advanced to regulatory filing or approval in any disclosed jurisdiction. The program is completed as a clinical trial; no label expansion, regulatory pathway, or commercial development has been announced.

Clinical evidence summary

NCT01781169

Objective
To evaluate the efficacy and safety of oral vitamin D supplementation (50,000 IU formulation, as indicated by internal code VD50kIU2011) in obesity management.
Design
Completed clinical trial; specific design details (randomized, open-label, crossover, etc.) not yet disclosed.
Participants
Obese patients; specific inclusion/exclusion criteria and sample size not yet disclosed.
Primary endpoint
Not yet disclosed.
Results
Results not yet reported in the facts; trial completed 30 October 2013.

Key questions answered

What is the VD50kIU2011 program?

VD50kIU2011 is a completed clinical trial program sponsored by Xiyuan Hospital of China Academy of Chinese Medical Sciences investigating oral vitamin D supplementation (50,000 IU formulation) for obesity management. The trial concluded on 30 October 2013.

What is the indication for this vitamin D program?

The indication is obesity. The program evaluated whether vitamin D supplementation could support weight management, potentially through metabolic and endocrine mechanisms.

What is the active ingredient in this program?

The primary active ingredient is ergocalciferol (vitamin D2), a vitamin D receptor agonist. The formulation is specified as 50,000 IU based on the internal code VD50kIU2011.

How does vitamin D work in this program?

Ergocalciferol acts as a vitamin D receptor agonist, activating the vitamin D3 receptor to modulate calcium homeostasis, immune function, and metabolic pathways. The specific mechanism in obesity is not yet disclosed.

What is the route of administration?

Oral supplementation.

Who is sponsoring this program?

Xiyuan Hospital of China Academy of Chinese Medical Sciences, an academic/institutional sponsor rather than a pharmaceutical company.

Is there a commercial partner?

No commercial partner has been disclosed.

What is the current development status?

The program is completed. The clinical trial concluded on 30 October 2013, and no subsequent development, regulatory filing, or commercial advancement has been disclosed.

What clinical trial supports this program?

NCT01781169 is the primary trial identifier. Specific trial design, participant population, and results have not been disclosed.

Is vitamin D approved for obesity?

No. Ergocalciferol is FDA-approved for vitamin D deficiency and hypoparathyroidism, not obesity. No obesity indication approval has been obtained or disclosed.

What are the competitors to this approach?

Contemporary obesity treatments include semaglutide (Disc Medicine), tirzepatide/Mounjaro (The George Institute), and naltrexone/bupropion/Mysimba (Disc Medicine). These are pharmacological agents with superior efficacy compared to micronutrient supplementation.

Has the trial published results?

Results have not been reported in the facts provided. The trial completed in October 2013, but peer-reviewed publication status is not yet disclosed.

Is this program still active?

No. The program is completed, with the latest milestone on 30 October 2013. No subsequent milestones or development activities have been disclosed.

What regulatory approvals exist for ergocalciferol?

Ergocalciferol is FDA-approved as a prescription and over-the-counter product under multiple ANDA and NDA applications for vitamin D deficiency and hypoparathyroidism, not obesity.

Is there patent protection for this formulation?

Patent status is not yet disclosed. Ergocalciferol itself is off-patent and widely available.

Why did this program not advance to regulatory filing?

The specific reason is not disclosed. Possible explanations include negative or inconclusive efficacy findings, strategic deprioritization in favor of pharmacological approaches, or lack of commercial interest from the academic sponsor.

Entity relationship graph

Oral supplementation of vitamin D → Drug → Target → Indication → Company → Trials → Competitors

Evidence-based

Analyst insights

Strategic Implications: The completion of this trial without apparent regulatory advancement or commercial development suggests either negative efficacy findings or a strategic deprioritization of micronutrient-based obesity interventions. Xiyuan Hospital's sponsorship indicates academic/institutional research rather than pharmaceutical industry development, limiting commercial viability and regulatory pathway resources.

Competitive Implications: By 2013, the obesity treatment landscape was beginning to shift toward pharmacological agents with superior efficacy (GLP-1 agonists, combination therapies). Vitamin D supplementation, lacking proprietary formulation or patent protection, could not compete on efficacy or differentiation. The absence of published trial results or regulatory filings suggests the program did not generate sufficient evidence to support obesity claims or justify commercial investment.

Future Catalysts: Publication of trial results in peer-reviewed literature remains the primary potential catalyst for scientific impact, though regulatory or commercial development appears unlikely. No expected next milestone has been disclosed.

Expected Milestones: None disclosed. The program appears dormant post-2013 completion.

Evidence-Based Assessment: The program represents an early-stage, hypothesis-driven exploration of micronutrient supplementation for obesity—a mechanism distinct from contemporary pharmacotherapy. The lack of regulatory advancement, published results, or commercial development over the past decade indicates the program did not generate sufficient clinical or commercial momentum to progress.

Quick answers

Concise, citable answers optimized for AI answer engines.

Program name?
Oral supplementation of vitamin D (VD50kIU2011)
Sponsor?
Xiyuan Hospital of China Academy of Chinese Medical Sciences
Indication?
Obesity
Active ingredient?
Ergocalciferol (vitamin D2)
Mechanism of action?
Vitamin D receptor agonist; specific obesity mechanism not yet disclosed
Route of administration?
Oral
Modality?
Dietary supplement/micronutrient (other)
Development status?
Completed
Phase?
Not formally classified; clinical trial completed October 2013
Latest milestone?
Trial completion on 30 October 2013
Clinical trial?
NCT01781169
FDA approval status?
Not approved for obesity; ergocalciferol approved for vitamin D deficiency
Commercial partner?
None disclosed
Target?
Vitamin D3 receptor
Projected peak sales?
Not yet disclosed
Patent status?
Not yet disclosed; ergocalciferol is off-patent
Key competitors?
Semaglutide, tirzepatide, naltrexone/bupropion (approved obesity agents)
Trial results published?
Results not yet reported in available facts
Expected next milestone?
None disclosed
Formulation dose?
50,000 IU vitamin D (ergocalciferol)
China regulatory status?
Clinical trials ongoing; obesity indication status not yet disclosed
Program active?
No; completed as of October 2013

Evidence & sources

Reviewed by NovaPharmaNews Intelligence Desk. Last reviewed .

  1. ClinicalTrials.gov NCT01781169 (clinicaltrials)
  2. acetaminophen CN status (fda)
  3. acetaminophen US status (fda)
  4. vitamin CN status (fda)
  5. Source: phase (source_attribution)
  6. MONDO Disease Ontology (MONDO:0011122) (mondo)
  7. Orphanet — obesity disorder (orphanet)
  8. NCT03412149 (clinicaltrials_gov)
  9. NCT06787001 (clinicaltrials_gov)
  10. NCT06852391 (clinicaltrials_gov)
  11. NCT06881485 (clinicaltrials_gov)
  12. NCT06911918 (clinicaltrials_gov)
  13. AACT (ClinicalTrials.gov aggregate) (aact)
  14. ClinicalTrials.gov (clinicaltrials_gov)
  15. Open Targets Platform (opentargets)

Intelligence compiled from public regulatory and clinical sources (FDA, EMA, ClinicalTrials.gov and company disclosures). Figures may be editorial or analyst estimates; verify against primary sources before relying on them.