Treating Cancer with High Dose (IV or liposomal) Vitamin C, and Vit C as Effective Adjunct Treatment or Combination Treatment

Documentation of Effectiveness

Curing the Incurable: Vitamin C, Cancer, Infectious Diseases, and Toxins , 3rd Edition Paperback – August 1, 2011;  by  MD JD Thomas E Levy  

He quickly found the medical journals were filled with thousands of studies and articles about vitamin C. Many of them reported similarly dramatic results with a myriad of diseases and other difficult medical conditions. Dr. Levy knew that this was information that all his colleagues needed. Consequently, he was compelled to spend the next four years researching and writing  Curing the Incurablevy  has taken great care to research, document, and report the vital truths about vitamin C — he cites over 1,200 scientific references.

Curing the Incurable   provides the information you need to most effectively use vitamin C to:

·  Prevent, cure, reverse and/or greatly improve a large list of health conditions.

·  Cut your mortality risk (from all causes) by as much as 50%.

·  Boost your immune system and energy levels to optimum levels.

Optimize blood and intracellular levels of vitamin C, & Dramatically increase bio-availability (up to 800% or more) without increasing your dose size. 

Dr. Thomas Levy: IV Vitamin C Can Reverse Cancer and Infections - The Health Show; DVD,   https://www.amazon.com/Dr-Thomas-Levy-Vitamin-Infections/dp/B01B29TXL4

 

Vitamin C: The Real Story , the Remarkable and Controversial Healing Factor- Paperback – October 23, 2015; by  Steve Hickey  PhD,  Andrew W. Saul   PhD

You will see that mega doses of vitamin C have proven to be an effective antibiotic, a nontoxic anticancer agent , and also a treatment for heart disease.

 

Hidden Epidemic: Silent Oral Infections Cause Most Heart Attacks and Breast Cancers , September  2017 .

Stop America's #1 Killer 2nd ed. Edition by  MD JD Levy  (Author),  MD Julian Whitaker  (Foreword).    ( Most  heart disease is a reversable arterial scurvy)

Anticancer Res.  2019 Feb;39(2):751-758.  doi : 10.21873/anticanres.13172.

 

Effect of High-dose Vitamin C Combined with Anti-cancer Treatment on Breast Cancer Cells.

Lee SJ 1,2 Jeong  JH 1,3 Lee IH 1,2 Lee J 1,4 Jung JH 1,4 Park HY 5,4 Lee DH 6 Chae YS 5,2 .

BACKGROUND/AIM: 

The anti-cancer effect of high doses of intravenous vitamin C (high-dose vitamin C) remains controversial despite growing evidence that high-dose vitamin C exerts anti-tumorigenic activity by increasing the amount of reactive oxygen species in cancer cells without meaningful toxicities. Therefore, this study attempted to demonstrate the in vitro anti-cancer activity of high-dose vitamin C in combination with conventional treatment in breast cancer.

MATERIALS AND METHODS: 

The pro-apoptotic effects of high-dose vitamin C (1.25 to 20 mM) with or without anti-cancer agents ( eribulin  mesylate, tamoxifen,  fulvestrant , or trastuzumab) were estimated using an MTT assay to measure the cell viability of a variety of breast cancer cell lines (MCF7, SK-BR3, and MDA-MB-231), as well as normal breast epithelial cells (MCF10A).

RESULTS

High-dose vitamin C (≥10 mM) significantly decreased cell viability of all breast cancer cell lines, particularly of MCF-7 cells.  The catalase activities of MCF7 and MDA-MD-231 cells were also lower than those of MCF10A cells. Moreover, cell viability of both MCF7 and MDA-MD-231 cells was decreased further when combining high-dose vitamin C and  eribulin  mesylate, and this was also true for MCF-7 cells when combining high-dose vitamin C with tamoxifen or  fulvestrant  and for SK-BR3 cells when combining high-dose vitamin C with trastuzumab in comparison with chemotherapy or endocrine therapy alone.

CONCLUSION: 

Combining high-dose vitamin C with conventional anti-cancer drugs can have therapeutic advantages against breast cancer cells.


Send to

Med Hypotheses.  2019 Jan;122:8-9.  doi : 10.1016/j.mehy.2018.10.006.  Epub  2018 Oct 11.

On infusion of high-dose ascorbate in treating cancer: Is it time for N-acetylcysteine pretreatment to enhance susceptibility and to lower side effects?

Valachová  K 1 Juránek  I 2 Rapta  P 3 Valent I 4 Šoltés  L 2 .

Author information

Abstract

Ascorbate administered intravenously gives a high plasma concentration of this drug. Clinical trials with pancreatic carcinoma patients revealed their prolonged survival if treated with intravenous ascorbate. On the other hand, high plasma ascorbate concentration leads to severe side effects, such as nephrotoxicity. In the present paper, we advocate to lower intravenous ascorbate dosage along with monothiol  N-acetylcysteine pretreatment due to anticipation of the same therapeutic effect but less or none of side effects . We describe in detail molecular mechanism of ascorbate action to be potentiated by N-acetylcysteine, as observed under in vitro conditions. Providing further arguments, we believe that the same mechanism may be employed in vivo.

Hidden Epidemic: Silent Oral Infections Cause Most Heart Attacks and Breast Cancers   Kindle Edition   by  MD JD Levy  

PubMed   High dose Vitamin C & Cancer (hundreds of studies)   https://www.ncbi.nlm.nih.gov/pubmed/?term=high+dose+vitamin+C+cancer

https://www.ncbi.nlm.nih.gov/pubmed/?term=high+dose+ascorbate+cancer

https://www.ncbi.nlm.nih.gov/pubmed/?term=vitamin+c+cancer


Life Sci.
 2019 Jul 12:116657.  doi : 10.1016/j.lfs.2019.116657. [ Epub  ahead of print]

High doses of sodium ascorbate interfere with the expansion of glioblastoma multiforme cells in vitro and in vivo.

Ryszawy D 1 Pudełek M 2 Catapano J 2 Ciarach M 3 Setkowicz Z 3 Konduracka E 4 Madeja Z 2 Czyż J 5 .

Author information

Abstract

AIMS: 

Constant development of chemotherapeutic strategies has considerably improved the efficiency of tumor treatment. However, adverse effects of chemotherapeutics enforce premature treatment cessation, which leads to the tumor recurrence and accelerated death of oncologic patients. Recently, sodium ascorbate (ASC) has been suggested as a promising drug for the adjunctive chemotherapy of glioblastoma multiforme (GBM) and prostate cancer (PC). To estimate whether ASC can interfere with tumor recurrence between the first and second-line chemotherapy, we analyzed the effect of high ASC doses on the expansion of cells in vitro and in vivo.

MAIN METHODS: 

Brightfield microscopy-assisted approaches were used to estimate the effect of ASC (1-14 mM) on the morphology and invasiveness of human GBM, rat PC and normal 3T3 cells, whereas cytostatic/pro-apoptotic activity of ASC was estimated with flow cytometry. These assays were complemented by the in vitro  CellROX -assisted analyses of intracellular oxidative stress and in vivo estimation of GBM tumor invasion.

KEY FINDINGS: 

ASC considerably decreased the proliferation and motility of GBM and PC cells. This effect was accompanied by intracellular ROS over-production and necrotic death of tumor cells , apparently resulting from their " autoschizis ". In vivo studies demonstrated the retardation of GBM tumor growth and invasion in the rats undergone intravenous ASC administration, in the absence of detectable systemic adverse effects of ASC.

SIGNIFICANCE: 

Our data support previous notions on anti-tumor activity of high ASC doses.  However,  autoschizis -related cell responses to ASC indicate that its application in human adjunctive tumor therapy should be considered with caution.


Nutrients.
 2019 Apr 28;11(5).  pii : E977.  doi : 10.3390/nu11050977.

The Effect of Vitamin C (Ascorbic Acid) in the Treatment of Patients with Cancer: A Systematic Review.

van  Gorkom  GNY 1 Lookermans  EL 2 Van  Elssen  CHMJ 3 Bos GMJ 4 .

Author information

Abstract

Many cancer patients on intensive chemotherapy lack vitamin C. Vitamin C stimulates the production and activation of immune cells, so perhaps supplementation could be used to improve the immunity in those patients. This review assesses the effectiveness and safety of vitamin C administration in cancer. The PubMed and EMBASE databases were searched and all study designs except for phase I studies, and case reports were included in this review. A total of 19 trials were included. In only 4 trials randomization was used to determine if patients received vitamin C or a placebo. The result of this review does not prove that there is a clinically relevant positive effect of vitamin C supplementation in cancer patients in general on the overall survival, clinical status, quality of life (QOL) and performance status (PS ), since the quality of the studies published is low. Interventions and patient groups are very diverse, hence an effect in some patient groups is possible. There seems to be a  better effect with intravenous than oral administration.  Nevertheless, treatment with vitamin C is safe with minimal side effects. Thereby, we think it is safe to examine the effects of vitamin C on specific groups of patients in a randomized controlled setting.



Int J Mol Sci.
 2018 Sep 13;19(9).  pii : E2752.  doi : 10.3390/ijms19092752.

Ascorbic Acid in Colon Cancer: From the Basic to the Clinical Applications.

El  Halabi  I 1 Bejjany  R 2 Nasr R 3 Mukherji D 4 Temraz  S 5 Nassar FJ 6 El  Darsa  H 7 Shamseddine  A 8 .

Author information

Abstract

Given the safety and potential benefits of intravenous ascorbic acid (AA) administration in cancer patients, there is merit in further exploring this therapeutic concept. In this review, we discuss the potential benefits of intravenous AA administration on colorectal  cancer  and we specifically focus on its effect on glycolysis in mutant and wild type  RAS . We perform a PubMed and Ovid MEDLINE search using ascorbic acid, intravenous vitamin C,  KRAS  mutation,  BRAF  mutation and colorectal cancer (CRC) as keywords. At the cellular level, colorectal cancer cells undergo a metabolic shift called the Warburg effect to allow for more glucose absorption and utilization of glycolysis. This shift also allows AA to enter which leads to a disruption in the Warburg effect and a shutdown of the downstream  KRAS pathway  in mutated  KRAS  colon cancer cells.  At the clinical level, AA is associated with  tumour  regression in advanced disease and improved tolerability and side effects of standard therapy. Based on these findings, we conclude that further clinical trials are needed on a larger scale to examine the therapeutic benefits of AA in colon cancer.


Antioxidants (Basel).
 2018 Aug 30;7(9).  pii : E115.  doi : 10.3390/antiox7090115.

The Use of Intravenous Vitamin C as a Supportive Therapy for a Patient with Glioblastoma Multiforme.

Baillie N 1 Carr  AC 2 Peng S 3 .

Author information

Abstract

Glioblastoma multiforme is a  high grade  malignant brain  tumour  with a poor prognosis. Here we report the case of a woman with glioblastoma who lived for over four years from diagnosis (median survival 12 months and 2% survival for three years), experiencing good quality of life for most of that time. She underwent initial debulking craniotomy, radiotherapy and chemotherapy, as well as having intravenous vitamin C infusions 2 3 times weekly over the four years from diagnosis. Her progress was monitored by blood tests, regular  computerisedtomography (CT) and magnetic resonance imaging (MRI) scans, clinical reviews and European Organization for the Research and Treatment of Cancer quality of life questionnaires (EORTC QLQ C30).  Our case report highlights the benefits of intravenous vitamin C as a supportive therapy for patients with glioblastoma.


Cancer  Manag  Res.
 2018 Jul  13;10:2003 -2018.  doi : 10.2147/CMAR.S161824.  eCollection  2018.

Evidence-based complementary treatment of pancreatic cancer: a review of adjunct therapies including paricalcitol, hydroxychloroquine, intravenous vitamin C, statins, metformin, curcumin, and aspirin.

Bigelsen  S 1 .

Author information

Abstract

Despite new and exciting research and renewed optimism about future therapy, current statistics of survival from pancreatic cancer remains dismal. Patients seeking alternative or complementary treatments should be warned to avoid the hype and instead look to real science. A variety of relatively safe and inexpensive treatment options that have shown success in preclinical models and/or retrospective studies are currently available. Patients require their physicians to provide therapeutic guidance and assistance in obtaining and administrating these various therapies. Paricalcitol, an analog of vitamin D, has been shown by researchers at the Salk Institute for Biological Studies to break though the protective stroma surrounding tumor cells. Hydroxychloroquine has been shown to inhibit autophagy, a process by which dying cells recycle injured organelles and internal toxins to generate needed energy for survival and reproduction.  Intravenous vitamin C creates a toxic accumulation of hydrogen peroxide within cancer cells, hastening their death . Metformin inhibits mitochondrial oxidative metabolism utilized by cancer stem cells. Statins inhibit not only cholesterol but also other factors in the same pathway that affect cancer cell growth, protein synthesis, and cell cycle progression.  A novel formulation of curcumin may prevent resistance to chemotherapy and inhibit pancreatic cancer cell proliferation.  Aspirin therapy has been shown to prevent pancreatic cancer and may be useful to prevent recurrence. These therapies are all currently available and are reviewed in this paper with emphasis on the most recent laboratory research and clinical studies.


Antioxidants (Basel).
 2018 Jul 12;7(7).  pii : E89.  doi : 10.3390/antiox7070089.

Systematic Review of Intravenous Ascorbate in Cancer Clinical Trials.

Nauman G 1 Gray JC 2 Parkinson R 3 Levine M 4 Paller  CJ 5 .

Author information

Abstract

BACKGROUND: 

Ascorbate (vitamin C) has been evaluated as a potential treatment for cancer as an independent agent and in combination with standard chemotherapies. This review assesses the evidence for safety and clinical effectiveness of intravenous (IV) ascorbate in treating various types of cancer.

METHODS: 

Single arm and randomized Phase I/II trials were included in this review. The PubMed, MEDLINE, and Cochrane databases were searched. Results were screened by three of the authors (GN, RP, and CJP) to determine if they met inclusion criteria, and then summarized using a narrative approach.

RESULTS: 

A total of 23 trials involving 385 patients met the inclusion criteria. Only one trial, in ovarian cancer, randomized patients to receive vitamin C or standard of care (chemotherapy). That trial reported  an 8.75 month increase in progression-free survival (PFS) and an improved trend in overall survival (OS) in the vitamin C treated arm .

CONCLUSION: 

Overall , vitamin C has been shown to be safe in nearly all patient populations, alone and in combination with chemotherapies . The promising results support the need for randomized placebo-controlled trials such as the ongoing placebo-controlled trials of vitamin C and chemotherapy in prostate cancer.


NPJ Precis Oncol.
 2018 Jan 8;2(1):1.  doi : 10.1038/s41698-017-0044-8.  eCollection  2018.

Vitamin C preferentially kills cancer stem cells in hepatocellular carcinoma via SVCT-2.

Lv  H #1 Wang C #1,2 Fang T #1 Li T 1 Lv  G 1,3 Han Q 1 Yang W 1,3 Wang H 1,3,4 .

Author information

Abstract

Vitamin C (L-ascorbic acid, ascorbate, VC) is a potential chemotherapeutic agent for cancer patients. However, the anti-tumor effects of pharmacologic VC on hepatocellular carcinoma (HCC) and liver cancer stem cells (CSCs) remain to be fully elucidated. Panels of human HCC cell lines as well as HCC patient-derived xenograft (PDX) models were employed to investigate the anti-tumor effects of pharmacologic VC. The use of VC and the risk of HCC recurrence were examined retrospectively in 613 HCC patients who received curative liver resection as their initial treatment. In vitro and in vivo experiments further demonstrated that clinically achievable concentrations of VC induced cell death in liver cancer cells and the response to VC was correlated with sodium-dependent vitamin  Ctransporter  2 (SVCT-2) expressions. Mechanistically, VC uptake via SVCT-2 increased intracellular ROS, and subsequently caused DNA damage and ATP depletion, leading to cell cycle arrest and apoptosis. Most importantly, SVCT-2 was highly expressed in liver CSCs, which promoted their self-renewal and rendered them more sensitive to VC. In HCC cell lines xenograft models, as well as in PDX models, VC dramatically impaired tumor growth and eradicated liver CSCs. Finally, retrospective cohort study showed that intravenous VC use was linked to improved disease-free survival (DFS) in HCC patients (adjusted HR = 0.622, 95% CI 0.487 to 0.795,  p  < 0.001). Our data highlight that  pharmacologic VC can effectively kill liver cancer cells and preferentially eradicate liver CSCs, which provide further evidence supporting VC as a novel therapeutic strategy for HCC treatment.


Integr
  Cancer   Ther .
 2018 Sep;17(3):912-920.  doi : 10.1177/1534735418775809.  Epub  2018 May 17.

Retrospective Evaluation of Clinical Experience  With  Intravenous Ascorbic Acid in Patients With Cancer.

Bazzan  AJ 1 Zabrecky  G 1 Wintering N 1 Newberg AB 1 Monti DA 1 .

Author information

Abstract

BACKGROUND: 

Intravenous   ascorbic acid   (IV AA) has been used extensively in cancer patients throughout the United States. Currently, there are limited data on the safety and clinical effects of IV AA. The purpose of this study was to expand the current literature using a retrospective analysis of adverse events and symptomatic changes of IV AA in a large sample of cancer patients.

METHODS: 

We conducted a retrospective chart review of all patients receiving IV AA for cancer at the Thomas Jefferson University Hospital over a 7-year period. We assessed all reports of adverse events, laboratory findings, and hospital or emergency department admissions. We also reviewed quality-of-life data, including fatigue, nausea, pain, appetite, and mood.

RESULTS: 

There were 86 patients who received a total of 3034 doses of IV AA ranging from 50 to 150g. In all, 32 patients received only ascorbic acid as part of their cancer management (1197 doses), whereas 54 patients received ascorbic acid in conjunction with chemotherapy (1837 doses). The most common adverse events related to ascorbic acid were temporary nausea and discomfort at the injection site. All events reported in the ascorbic acid alone group were associated with less than 3% of the total number of infusions.  Patients, overall, reported improvements in fatigue, pain, and mood while receiving ascorbic acid.

CONCLUSIONS: 

The results of this retrospective analysis support the growing evidence that  IV AA is generally safe and well tolerated in patients with  cancer, and  may be useful in symptom management and improving quality of life.


Anticancer Drugs.
 2018 Apr;29(4):373-379.  doi : 10.1097/CAD.0000000000000603.

Treatment of pancreatic cancer with intravenous vitamin C: a case report.

Drisko  JA 1 Serrano OK 2 Spruce LR 3 Chen Q 4 Levine M 5 .

Author information

Abstract

Pancreatic ductal adenocarcinoma (PDA) has a dismal prognosis and is often discovered at an advanced stage with few therapeutic options. Current conventional regimens for PDA are associated with significant morbidity, decreased quality of life, and a considerable financial burden. As a result, some patients turn to integrative medicine therapies as an alternate option after a diagnosis of PDA. Intravenous pharmacologic ascorbic acid (PAA) is one such treatment. The use of PAA has been passionately debated for many years, but more recent rigorous scientific research has shown that there are significant blood concentration differences when ascorbic acid is given parenterally when compared to oral dosing. This pharmacologic difference appears to be critical for its role in oncology. Here, we report the use of PAA in a patient with poorly differentiated stage IV PDA as an exclusive chemotherapeutic regimen. The  patient survived nearly 4 years after diagnosis, with PAA as his sole treatment, and he achieved objective regression of his disease.  He died from sepsis and organ failure from a bowel perforation event. This case illustrates the possibility of PAA to effectively control tumor progression and serve as an adjunct to standard of care PDA chemotherapy regimens. Our patient's experience with PAA should be taken into consideration, along with previous research in cell, animal, and clinical experiments to design future treatment trials.


Clin Exp Metastasis.
 2018 Feb;35(1-2):37-51.  doi : 10.1007/s10585-018-9876-z.  Epub  2018 Feb 2.

Pharmacologic ascorbate (P- AscH - ) suppresses hypoxia-inducible Factor-1α (HIF-1α) in pancreatic adenocarcinoma.

Wilkes JG 1,2 O'Leary BR 1,2 Du J 1,2 Klinger AR 1 Sibenaller  ZA 1 Doskey  CM 1 Gibson-Corley KN 3,4 Alexander MS 1,2 Tsai S 5 Buettner GR 1,4 Cullen JJ 6,7,8,9,10 .

Author information

1

Department of Radiation Oncology, University of Iowa Carver College of Medicine, Iowa City, IA, USA.

2

Department of Surgery, University of Iowa Carver College of Medicine, Iowa City, IA, USA.

3

Department of Pathology, University of Iowa Carver College of Medicine, Iowa City, IA, USA.

4

Holden Comprehensive Cancer Center, Iowa City, IA, USA.

5

The Medical College of Wisconsin, Milwaukee, WI, USA.

6

Department of Radiation Oncology, University of Iowa Carver College of Medicine, Iowa City, IA, USA. joseph-cullen@uiowa.edu.

7

Department of Surgery, University of Iowa Carver College of Medicine, Iowa City, IA, USA. joseph-cullen@uiowa.edu.

8

Holden Comprehensive Cancer Center, Iowa City, IA, USA. joseph-cullen@uiowa.edu.

9

Veterans Affairs Medical Center, Iowa City, IA, USA. joseph-cullen@uiowa.edu.

10

University of Iowa Hospitals and Clinics, 1528 JCP, 200 Hawkins Drive, Iowa City, IA, 52242, USA. joseph-cullen@uiowa.edu.

Abstract

HIF-1α is a transcriptional regulator that functions in the adaptation of cells to hypoxic conditions; it strongly impacts the prognosis of patients with cancer. High-dose, intravenous, pharmacological ascorbate (P- AscH - ), induces cytotoxicity and oxidative stress selectively in cancer cells by acting as a pro-drug for the delivery of hydrogen peroxide (H 2 O 2 ); early clinical data suggest improved survival and inhibition of metastasis in patients being actively treated with P- AscH - . Previous studies have demonstrated that activation of HIF-1α is necessary for P- AscH - sensitivity. We hypothesized that  pancreatic cancer (PDAC) progression and metastasis could be  be  targeted by P- AscH -   via H 2 O 2 -mediated inhibition of HIF-1α stabilization. Our study demonstrates an oxygen- and prolyl hydroxylase-independent regulation of HIF-1α by P- AscH - . Additionally , P- AscH -   decreased VEGF secretion in a dose-dependent manner that was reversible with catalase, consistent with an H 2 O 2 -mediated mechanism.   Pharmacological and genetic manipulations of HIF-1α did not alter P- AscH - -induced cytotoxicity. In vivo,  P- AscH - inhibited tumor growth and VEGF expression.   We conclude that P- AscH -   suppresses the levels of HIF-1α protein in hypoxic conditions through a post-translational mechanism. These findings suggest potential new therapies specifically designed to inhibit the mechanisms that drive metastases as a part of PDAC treatment.


Leuk Res.
 2018  Mar;66:1 -7.  doi : 10.1016/j.leukres.2017.12.009.  Epub  2018 Jan 2.

The synergy of Vitamin C with decitabine activates TET2 in leukemic cells and significantly improves overall survival in elderly patients with acute myeloid leukemia.

Zhao H 1 Zhu H 2 Huang J 3 Zhu Y 2 Hong M 2 Zhu H 2 Zhang J 3 Li S 3 Yang L 3 Lian Y 3 Wang S 2 Mao J 3 Chen Y 2 Li J 2 Qian S 4 .

Author information

Abstract

BACKGROUND: 

Decitabine is widely used in the treatment of acute myeloid leukemia (AML) in elderly patients. Low-dose Vitamin C has also been indicated to induce DNA demethylation at the cellular level. However, little is known whether low-dose Vitamin C has a synergistic effect with decitabine in clinic.

METHODS: 

The effect of combined low-dose Vitamin C and decitabine on cell proliferation, the cell cycle, apoptosis and the expression level and activity of TET2 was investigated in HL60 and NB4 human leukemic cells. Additionally, we analyzed the clinical outcomes of 73 elderly AML patients who received A-DCAG (intravenous Vitamin C [IVC] plus DCAG [n = 39]) or DCAG (n = 34) treatment.

RESULTS: 

We found that low-dose Vitamin C and decitabine has a synergistic efficacy on proliferation, apoptosis, TET2 expression and activity, compared to drug-alone treatment in HL60 and NB4 cell lines in vitro. In clinic, feasibility and safety evaluations revealed that patients who received A-DCAG regimen have a higher complete remission (CR) rate than those who received the DCAG regimen (79.92% vs. 44.11%; P = 0.004) after one cycle of chemotherapy. The median overall survival (OS) was better in the A-DCAG group compared with the DCAG group (15.3 months vs. 9.3 months, P = 0.039). Patients with adverse cytogenetics did benefit from CR. There was no clinically significant additional toxicity observed with the addition of IVC.

CONCLUSION: 

On the basis of these results , the addition of IVC at low doses to DCAG appeared to improve CR and prolong OS, compared with DCAG, in elderly patients with AML.


Integr  Cancer  Ther .
 2018 Sep;17(3):986-993.  doi : 10.1177/1534735417747984.  Epub  2017 Dec 19.

The Long-Term Survival of a Patient  With  Stage IV Renal Cell Carcinoma Following an Integrative Treatment Approach Including the Intravenous α-Lipoic Acid/Low-Dose Naltrexone Protocol.

Berkson  BM 1,2 Calvo  Riera  F 3 .

Author information

Abstract

In this case report, we describe the treatment of a 64-year-old male patient diagnosed with metastatic renal cell carcinoma (RCC) in June of 2008. In spite of a left nephrectomy and the standard oncological protocols, the patient developed a solitary left lung metastasis that continued to grow. He was informed that given his diagnosis and poor response to conventional therapy, any further treatment would, at best, be palliative. The patient arrived at the Integrative Medical Center of New Mexico in August of 2010. He was in very poor health, weak, and cachectic. An integrative program-developed by one of the authors using intravenous (IV) α-lipoic acid, IV vitamin C, low-dose naltrexone, and  hydroxycitrate , and a healthy life style program-was initiated. From August 2010 to August 2015, the patient's RCC with left lung metastasis was followed closely using computed tomography and positron emission tomography/computed tomography imaging. His most recent positron emission tomography scan demonstrated no residual increased glucose uptake in his left lung. After only a few treatments of IV α-lipoic acid and IV vitamin C, his symptoms began to improve, and the patient regained his baseline weight. His energy and outlook improved, and he returned to work. The patient had stable disease  with disappearance of the signs and symptoms of stage IV RCC, a full 9 years following diagnosis, with a gentle integrative program, which is essentially free of side effects.  As of  November 2017 the patient feels well and is working at his full-time job.

 


Send to

Sci Rep.  2017 Dec 7;7(1):17188.  doi : 10.1038/s41598-017-17568-8.

High Dose Parenteral Ascorbate Inhibited Pancreatic Cancer Growth and Metastasis: Mechanisms and a Phase I/ IIa  study.

Polireddy  K 1,2 Dong R 1,2 Reed G 1 Yu J 1,2 Chen P 1,2 Williamson S 3 Violet PC 4 Pessetto  Z 5 Godwin AK 5 Fan F 5 Levine M 4 Drisko  JA 6 Chen Q 7,8 .

Author information

Abstract

Pancreatic cancer is among the most lethal cancers with poorly tolerated treatments. There is increasing interest in using high-dose intravenous ascorbate (IVC) in treating this disease partially because of its low toxicity. IVC bypasses bioavailability barriers of oral ingestion, provides pharmacological concentrations in tissues, and exhibits selective cytotoxic effects in cancer cells through peroxide formation. Here, we further revealed its anti-pancreatic cancer mechanisms and conducted a phase I/ IIa  study to investigate pharmacokinetic interaction between IVC and gemcitabine. Pharmacological ascorbate induced cell death in pancreatic cancer cells with diverse mutational backgrounds. Pharmacological ascorbate depleted cellular NAD+ preferentially in cancer cells versus normal cells, leading to depletion of ATP and robustly increased α-tubulin acetylation in cancer cells. While ATP depletion led to cell death, over-acetylated tubulin led to inhibition of motility and mitosis. Collagen was increased, and  cancer cell epithelial-mesenchymal transition (EMT) was inhibited,   accompanied with inhibition in metastasis.  IVC was safe in patients and showed the possibility to prolong patient survival. There was no interference to gemcitabine pharmacokinetics by IVC administration. Taken together, these data revealed a multi-targeting mechanism of pharmacological ascorbate's anti-cancer action, with minimal toxicity, and provided guidance to design larger definitive trials testing efficacy of IVC in treating advanced pancreatic cancer.


Altern  Ther  Health Med.
 2019 Mar;25(2):42-45.

Brief Report: Stability and Chemical Characteristics of Injectable Ascorbic Acid for Patients  With  Cancer.

Monti DA Bazzan  AJ Zabrecky  G Newberg AB .

Abstract

CONTEXT: 

Intravenous   ascorbic acid   (IVAA) has been used extensively as part of the management plan for  cancerpatients  in various medical clinics throughout the United States. The current research team has evaluated its effectiveness in patients with cancer as part of an ongoing research program. However, no data are available that support the chemical stability of intravenously injectable ascorbic acid (AA) to ensure its safety and efficacy in that patient population. Its clinical use as well as its use in research conducted in US Food and Drug Administration-approved clinical trials require validation of its stability.

OBJECTIVE: 

The study intended to evaluate the chemical stability of the compounded IVAA that it prepares.

DESIGN: 

The research team conducted a stability analysis within a 6-h period, a period longer than the time required for most infusions, which typically take approximately 2 h. The study evaluated the stability of AA intravenous sets, which are compounded solutions for clinical or hospital use. The IVAA was prepared in sterile water, together with magnesium chloride ( MgCl ) and calcium gluconate ( CaGluc ) as buffers.

SETTING: 

The study took place at the Marcus Institute of Integrative Health at Thomas Jefferson University (Philadelphia, PA, USA).

OUTCOME MEASURES: 

The study was performed for 2 dosages of an infusion set: 75 g and 100 g of IVAA. Interval testing included pH, particulate matter by light obscuration, and high-performance liquid chromatography assay. Analyses were performed at baseline and at 2-, 4-, and 6-h test intervals.

RESULTS: 

The results demonstrated that IVAA remained highly stable throughout the 6-h period. It also passed the US Pharmacopeia's criteria for pH and particulates when used with a 0.2 µ filter.

CONCLUSIONS: 

These data suggest that  IVAA, when prepared with sterile water, in addition to  MgCl  and  CaGluc , is highly stable and safe to use in patients for up to 6 h after preparation.

 


Biochem   Biophys  Rep.
 2017 Apr  22;10:232 -236.  doi : 10.1016/j.bbrep.2017.04.014.  eCollection  2017 Jul.

2- O -α-D-Glucopyranosyl-l-ascorbic acid as an antitumor agent for infusion therapy.

Miura K 1 Tai A 1 .

Author information

Abstract

Ascorbic acid (AA) has been reported as a treatment for cancer patients. Intravenous (iv)  administration of high-dose AA increases plasma AA levels to pharmacologic concentrations and generates reactive oxygen species (ROS) to exert anti-tumor activity via enhancement of oxidative stress . However, AA is very unstable in aqueous solutions and it is impossible to preserve AA for a long period in a solution. 2- O -α-D-Glucopyranosyl-l-ascorbic acid (AA-2G), which is a glucoside derivative of AA, has been found to exhibit much higher stability than AA in aqueous solutions and it shows vitamin C activity after enzymatic hydrolysis to AA. To evaluate the effectiveness of AA-2G for cancer treatment, we examined the antitumor activity of AA-2G to murine colon carcinoma (colon-26) cells and in tumor-bearing mice. AA-2G did not show cytotoxicity to colon-26 cells, whereas AA exhibited a significant cytotoxic effect in a concentration-dependent manner. In colon-26 tumor-bearing mice, iv administration of high-dose AA-2G as well as that of AA significantly inhibited tumor growth. Experiments on the biodistribution and clearance of AA-2G in tumor-bearing mice showed that AA-2G was rapidly hydrolyzed to AA and exhibited significant antitumor activity. Treatment of tumor-bearing mice with AA-2G tended to increase plasma malondialdehyde level.  These results indicated that the antitumor activity of AA-2G was caused by ROS generated by AA released by rapid hydrolysis of AA-2G.


Exp  Ther  Med.
 2016 Nov;12(5):3058-3062.  Epub  2016 Sep 16.

In vitro   and  in vivo  assessment of high-dose vitamin C against murine tumors.

Wang G 1 Yin T 1 Wang Y 1 .

Author information

Abstract

Vitamin C is widely used in clinical settings and is well known for its safety. Previous studies have shown the efficacy of intravenous vitamin C; however,  intratumoral  delivery of vitamin C has yet to be attempted. In the present study, the biological effects of high-dose vitamin C on tumor cells were investigated  in vitro  by using the MTT assay and flow cytometry. When administered  in vitro ,   high-dose vitamin C inhibited the proliferation of murine colon and breast cancer cells, and induced tumor cell apoptosis Cytotoxicity of vitamin C was partially reversed by N- acetyl-cysteine at a relatively low dosage. In addition, synergistic anti-tumor effects of vitamin C and cisplatin were observed.  In vivo,  intratumoral  delivery of vitamin C delayed tumor growth in murine solid tumor models. Considering its low toxicity and availability, the present study indicates that vitamin C may be a novel therapeutic method for patients with advanced tumors.  chemotherapy drug cisplatin


Pain Res  Manag .
 2016;2016:9147279.  Epub  2016 Oct 30.

Effect of Intravenous High Dose Vitamin C on Postoperative Pain and Morphine Use after Laparoscopic Colectomy: A Randomized Controlled Trial.

Jeon Y 1 Park JS 2 Moon S 3 Yeo J 4 .

Author information

Abstract

Background and Objective . Vitamin C has antioxidant, neuroprotective, and neuromodulating effects. Recently, it showed antinociceptive effect as a result of the antioxidant properties. Therefore, we designed this study to assess the effect of intravenous vitamin C on opiate consumption and pain in patients undergoing laparoscopic colectomy.  Methods . A total of 100 patients were enrolled and allocated to receive 50 mg/kg vitamin C or placebo by  intravenousinfusion  immediately after induction of anesthesia. Morphine consumption and scores of  painwere assessed at 2, 6, and 24 h after completion of surgery.  Results . There were 97 patients included in the analysis. Patients who received vitamin C had higher plasma concentrations of vitamin C at the end of surgery, significantly lower morphine consumption at the 2 h after end of surgery, and significantly lower pain scores at rest during first 24 h postoperatively. There was no significant difference between groups in side effects, fatigue score, or pain score during cough.  Conclusion . This study shows  high dose vitamin C infusion decreased postoperative pain during the first 24 h and reduced morphine consumption in the early postoperative period.  Additional research needed to examine whether higher doses of vitamin C and longer infusion times can amplify these effects.


Redox Biol.
 2016  Dec;10:274 -284.  doi : 10.1016/j.redox.2016.10.010.  Epub  2016 Oct 28.

Tumor cells have decreased ability to metabolize H 2 O 2 : Implications for pharmacological ascorbate in cancer therapy.

Doskey  CM 1 Buranasudja  V 1 Wagner BA 2 Wilkes JG 3 Du J 3 Cullen JJ 4 Buettner GR 5 .

Author information

Abstract

Ascorbate ( AscH - ) functions as a versatile reducing agent. At pharmacological doses (P- AscH - ; [plasma  AscH - ] ≥≈20mM), achievable through intravenous delivery,  oxidation of P- AscH -   can produce a high flux of H 2 O 2   in tumors.   Catalase is the major enzyme for detoxifying high concentrations of H 2 O 2 . We hypothesize that sensitivity of tumor cells to P- AscH -   compared to normal cells is due to their  lower capacity to metabolize H 2 O 2 . Rate constants for removal of H 2 O 2   ( k cell ) and catalase activities were determined for 15 tumor and 10 normal cell lines of various tissue types. A differential in the capacity of cells to remove H 2 O 2   was revealed, with the  average  k cell  for normal cells being twice that of tumor cells.  The ED 50   (50%  clonogenicsurvival ) of P- AscH -   correlated directly with  k cell  and catalase activity.  Catalase activity could present a promising indicator of which tumors may respond to P- AscH - .


Am J Case Rep.
 2016 Oct  24;17:774 -781.

High-Dose Intravenous Vitamin C Treatment of a Child with Neurofibromatosis Type 1 and Optic Pathway Glioma: A Case Report.

Mikirova  N 1 Hunnunghake  R 2 Scimeca  RC 1 Chinshaw  C 3 Ali F 3 Brannon C 2 Riordan N 4 .

Author information

Abstract

BACKGROUND In neurofibromatosis type 1 (NF1) disease, the loss of the tumor suppressor function of the neurofibromin gene leads to proliferation of neural tumors. In children, the most frequently identified tumor is the optic pathway glioma. CASE REPORT We describe the case of a 5-year-old child who was diagnosed with NF1 and optic pathway tumor onset at the age of 14 months. Because of the tumor progression, chemotherapy with carboplatin and vincristine was prescribed at this early age and continued for one year. As the progression of disease continued after chemotherapy, the child, at the age of 2.8 years, was started on high-dose intravenous vitamin C (IVC) treatment (7-15 grams per week) for 30 months.  After 30 months, the results of IVC treatments demonstrated reduction and stabilization of the tumors in the optic chiasm, hypothalamus, and left optic nerve according to radiographic imaging. The right-sided optic nerve mass seen before IVC treatment disappeared by the end of the treatment . CONCLUSIONS This case highlights  the positive effects of treating NF1 glioma with IVC . Additional studies are necessary to evaluate the role of high-dose IVC in glioma treatment.


Free  Radic  Biol Med.
 2016  Oct;99:451 -462.  doi : 10.1016/j.freeradbiomed.2016.08.027.  Epub  2016 Aug 24.

Pharmacokinetic and anti-cancer properties of high dose ascorbate in solid  tumours  of ascorbate-dependent mice.

Campbell EJ 1 Vissers  MCM 2 Wohlrab  C 1 Hicks KO 3 Strother RM 4 Bozonet  SM 2 Robinson BA 5 Dachs  GU 6 .

Author information

Abstract

Despite recent evidence for an anti- tumour  role for high-dose ascorbate, potential mechanisms of action are still unclear. At mM concentrations that are achieved with high-dose intravenous administration, autoxidation of ascorbate can generate cytotoxic levels of H 2 O 2 . Ascorbate is also a required co-factor for the hydroxylases that suppress the transcription factor hypoxia-inducible factor (HIF-1). HIF-1 supports an aggressive  tumour  phenotype and is associated with poor prognosis, and previous studies have shown that optimizing intracellular ascorbate levels down-regulates HIF-1 activation. In this study we have simultaneously measured ascorbate concentrations and the HIF-1 pathway activity in  tumour  tissue following high dose ascorbate  administration, and  have studied  tumour  growth and physiology. Gulo -/-   mice, a model of the human ascorbate dependency condition, were implanted with syngeneic Lewis lung  tumours , 1g/kg ascorbate was administered into the peritoneum, and ascorbate concentrations were monitored in plasma, liver and  tumours . Ascorbate levels peaked within 30min, and although plasma and liver ascorbate returned to baseline within 16h,  tumour  levels remained elevated for 48h, possibly reflecting increased stability in the hypoxic  tumour  environment. The expression of HIF-1 and its target proteins was down-regulated with  tumour  ascorbate uptake. Elevated  tumour  ascorbate levels could be maintained with daily administration, and HIF-1 and vascular endothelial growth factor protein levels were reduced in these conditions.  Increased  tumour  ascorbate was associated with slowed  tumour  growth, reduced  tumour   microvessel  density and decreased hypoxia.  Alternate day administration of ascorbate resulted in lower  tumour  levels and did not consistently decrease HIF-1 pathway activity. Levels of sodium-dependent vitamin C transporters 1 and 2 were not clearly associated with ascorbate accumulation by murine  tumour  cells in vitro or in vivo. Our  results support the suppression of the hypoxic response by ascorbate as a plausible mechanism of action of its anti- tumour  activity,  and this may be useful in a clinical setting.


Med Sci  Monit .
 2016 Jan 3;22:14-25.

Modulation of Cytokines in Cancer Patients by Intravenous Ascorbate Therapy.

Mikirova  N 1 Riordan N 2 Casciari  J 3 .

Author information

Abstract

BACKGROUND: 

Cytokines play an important role in tumor angiogenesis and inflammation. There is evidence in the literature that high doses of ascorbate can reduce inflammatory cytokine levels in cancer patients. The objective of this study was to investigate the effect of treatment by intravenous vitamin C (IVC) on cytokines and tumor markers.

MATERIAL/METHODS: 

With the availability of protein array kits allowing assessment of many cytokines in a single sample, we measured 174 cytokines and additional 54 proteins and tumor markers in 12 cancer patients before and after a series of IVC treatments.

RESULTS: 

Presented results show  for our 12 patients the effect of treatment resulted in normalization of many cytokine levels.  Cytokines that were most consistently elevated prior to treatments included M-CSF-R, Leptin, EGF, FGF-6, TNF-α, β, TARC, MCP-1,4, MIP, IL-4, 10, IL-4, and TGF-β. Cytokine levels tended to decrease during the course of treatment. These include mitogens (EGF, Fit-3 ligand, HGF, IGF-1, IL-21R) and chemo-attractants (CTAC,  Eotaxin , E-selectin, Lymphotactin, MIP-1, MCP-1, TARC, SDF-1), as well as inflammation and angiogenesis factors (FGF-6, IL-1β, TGF-1).

CONCLUSIONS: 

We are able to show that  av.erage  z-scores for several inflammatory and angiogenesis promoting cytokines are positive, indicating that they are higher than averages for healthy controls, and that  their levels decreased over the course of treatment.  In addition,  serum concentrations of tumor markers decreased during the time period of IVC treatment and there were reductions in  cMyc  and Ras, 2 proteins implicated in being upregulated in cancer.


Integr
  Cancer   Ther .
 2016 Jun;15(2):197-204.  doi : 10.1177/1534735415622010.  Epub  2015 Dec 17.

Effects of High Doses of Vitamin C on Cancer Patients in Singapore: Nine Cases.

Raymond YC 1 Glenda CS 2 Meng LK 3 .

Author information

Abstract

Introduction Intravenous high-dose vitamin C therapy is widely used in naturopathic and integrative oncology; however, a study reviewing its effects has never been performed in Singapore. This article serves to document administration of supportive vitamin C therapy for cancer patients in Singapore.

METHODS: 

The clinical response of 9 cancer patients of differing stages to the regular administration of large doses (25-100 g/d) of intravenous vitamin C (IVC; ascorbic acid) is outlined. Tumor pathology and patient health were verified by doctors who do not practice vitamin C treatment.

RESULTS: 

Cases suggesting survival beyond prognosis, improvement in quality of life, safe coadministration with and improved tolerance of conventional therapy, and deterioration in clinical condition following withdrawal of vitamin C therapy are documented clinically . Some patients experience the  Jarisch-Herxheimer  reaction-the release of endotoxin from microorganism death resulting in pimples, fever, and body odor-for a few hours after the therapy, but these are resolved quickly with no lasting effects.

CONCLUSION: 

Randomized trials of IVC therapy are recommended because it  has minimal side effects and has shown promising results.

Curing the Incurable: Vitamin C, Infectious Diseases, and Toxins, 3rd Edition Paperback – August 1, 2011; by  MD JD Thomas E Levy  

He quickly found the medical journals were filled with thousands of studies and articles about vitamin C. Many of them reported similarly dramatic results with a myriad of diseases and other difficult medical conditions. Dr. Levy knew that this was information that all his colleagues needed. Consequently, he was compelled to spend the next four years researching and writing  Curing the Incurablevy  has taken great care to research, document, and report the vital truths about vitamin C — he cites over 1,200 scientific references.

Curing the Incurable   provides the information you need to most effectively use vitamin C to:

·   Prevent, cure, reverse and/or greatly improve a large list of health conditions.

·   Cut your mortality risk (from all causes) by as much as 50%.

·   Boost your immune system and energy levels to optimum levels.

Optimize blood and intracellular levels of vitamin C, & Dramatically increase bio-availability (up to 800% or more) without increasing your dose size. 

Dr. Thomas Levy: IV Vitamin C Can Reverse Cancer and Infections - The Health Show; DVD,   https://www.amazon.com/Dr-Thomas-Levy-Vitamin-Infections/dp/B01B29TXL4

Vitamin C: The Real Story, the Remarkable and Controversial Healing Factor Paperback – October 23, 2015; by  Steve Hickey  PhD,  Andrew W. Saul   PhD

You will see that mega doses of vitamin C have proven to be an effective antibiotic, a nontoxic anticancer agent, and also a treatment for heart disease.

 

Hidden Epidemic: Silent Oral Infections Cause Most Heart Attacks and Breast Cancers , was published in September of 2017.

Stop America's #1 Killer 2nd ed. Edition by  MD JD Levy  (Author),  MD Julian Whitaker  (Foreword).    ( Most  heart disease is a reversable arterial scurvy)

Hidden Epidemic: Silent Oral Infections Cause Most Heart Attacks and Breast Cancers   Kindle Edition   by  MD JD Levy  

The Toxic Tooth: How a root canal could be making you sick   (Kindle Edition );  

by  Robert  Kulacz   (Author),  MD JD Levy  (Author); foreword by Boyd Haley  Phd

What You Need to Know Before Undergoing a Root Canal Undergoing a root canal procedure isn't anyone's idea of a good time, but if one is necessary, we don't question its safety. According to Robert  Kulacz , DDS and Thomas E. Levy, MD, JD, we should. Here, they reveal the hidden dangers of root canals. Nobody looks forward to having a root canal. But if you're in constant discomfort because of an infected tooth, you'll willingly hop into the dentist's chair and open wide. Sure, you might worry about feeling pain during the procedure (or paying for it afterward), but beyond those concerns, there's really no reason to worry about undergoing this common outpatient procedure, right? Wrong. Robert  Kulacz , DDS and Thomas E. Levy, MD, JD, say that a root canal is actually a scientifically flawed and potentially dangerous procedure. "Instead of solving a problem, root canals introduce a steady stream of dangerous-and even deadly-toxins into your body," says Dr. Levy, co-author along with Dr.  Kulacz  of The Toxic Tooth: How a root canal could be making you sick. "Root canal-treated teeth are not sterile and contain pathogenic bacteria, which spread throughout the body and can initiate or worsen heart disease, lung disease, diabetes, osteoporosis, and even cancer."

https://www.amazon.com/s?k=thomas+levy+vitamin+c&gclid=EAIaIQobChMIvZvYx9Hz4wIVSFmGCh0hsA5yEAMYAiAAEgLBFPD_BwE&hvadid=177166317595&hvdev=c&hvlocphy=9011598&hvnetw=g&hvpos=1o2&hvqmt=e&hvrand=17462257267673753184&hvtargid=kwd-72493707154&hydadcr=15521_9752784&tag=googhydr-20&ref=pd_sl_65las1brw7_e

https://www.amazon.com/Toxic-Tooth-canal-could-making-ebook/dp/B00TZ9L1JQ/ref=sr_1_14?gclid=EAIaIQobChMIvZvYx9Hz4wIVSFmGCh0hsA5yEAMYAiAAEgLBFPD_BwE&hvadid=177166317595&hvdev=c&hvlocphy=9011598&hvnetw=g&hvpos=1o2&hvqmt=e&hvrand=17462257267673753184&hvtargid=kwd-72493707154&hydadcr=15521_9752784&keywords=thomas+levy+vitamin+c&qid=1565281519&s=gateway&sr=8-14