GenSpera’s Targeted “Death Carrot” Toxin in Trials for Two Cancers

XCONOMY

Top Stories in Texas

http://www.xconomy.com/texas/

GenSpera’s Targeted “Death Carrot” Toxin in Trials for Two Cancers

http://www.xconomy.com/texas/2014/03/27/gensperas-targeted-death-carrot-toxin-in-trials-for-two-cancers/

Bernadette Tansey 3/27/14

 

Craig Dionne has a record of experience in drug development and a lot of friends in the pharmaceutical industry. But when his friends first heard about the experimental drug he started working on some years ago, he says their initial reaction was alarm—to put it mildly.

“They told me I was a fool,” Dionne says affably. Dionne is CEO of San Antonio, TX-based GenSpera, which has now started a second round of early stage clinical trials on the experimental drug he took a chance on. He’s hoping the trials are about to show his friends he was right.

Back in the early 1990s, Dionne and his collaborators at Johns Hopkins University saw potential for a cancer drug in a highly potent toxin, thapsigargin, found in a common Mediterranean weed called Thapsia Garganica. You’ll find it described as the “death carrot’’ in online accounts.

Thapsigargin kills fast-growing cells. So far, so good; that’s a routine property of chemotherapy drugs. But the relative safety of classical chemotherapy agents rests on the fact that they’re more destructive to rapidly multiplying tumor cells than they are to slow-growing normal cells.

Thapsigargin doesn’t work that way—which initially made it alarming to Dionne’s friends. It’s an equal opportunity cell-killer.

“It can kill cells that grow slowly,” Dionne says. That makes it a threat to normal cells, unless a drug company can successfully tweak it. And Dionne saw a reason to try.

Like most normal cells, some cancer cells also grow slowly, such as those in tumors of the prostate. And such cancer cells can resist chemotherapy drugs that target fast-growing cells. Dionne and his collaborators at Johns Hopkins reasoned that thapsigargin might be an effective weapon against slow-growing tumor cells, if it could be modified to spare normal cells. The end result of their chemical tinkering is GenSpera’s experimental drug G-202, which has now moved into a second round of early stage clinical trials.

The compound was designed to allow the powerful toxin to move through the bloodstream in an inactive form until it’s released by an enzyme, PSMA, found at higher levels on the surface of certain tumor cells, Dionne says. He compares G-202 to a grenade with a pin ready to be pulled.

A molecule of G-202 contains a modified form of thapsigargin called 12ADT, which is linked to a small peptide. The effect of that peptide—a small chain of five amino acids—is to keep 12ADT soluble in the watery environment of the blood. More importantly, he peptide keeps the toxin inactive.

But when G-202 encounters a cell with the enzyme PSMA (prostate-specific membrane antigen) on its surface, the enzyme clips the peptide off the toxic 12ADT molecule. The toxin, now insoluble in water but highly soluble in fats, can sink through the lipid-rich outer membrane of a nearby cancer cell and start its deadly work.

Dionne says G-202 is similar to the new class of targeted cancer drugs called antibody-drug conjugates, which are also designed to deliver a toxin only to particular tumor cells. These drugs combine a toxin with an antibody engineered to bind to a specific molecule on the surface of a cancer cell. However, antibodies are large proteins whose unique amino acid sequences and folding patterns can help them fit selectively only with certain cell surface receptors.

Serotonin-producing cells develop early on in the ENS, and if this buy generic levitra development is affected, the second brain cannot form properly. You will be helped to prolong your erection in a more healthy levitra online devensec.com and natural way by this medicine. Sexual dysfunction is a common concern shared by many women. generic levitra cheap This levitra 20mg canada medicine may lead to allergic reaction in some individuals. By contrast, G-202‘s targeting agent, the small peptide, could theoretically be clipped away from its toxic payload by enzymes other than PSMA, Dionne says. If that happened, the toxin could be released in the vicinity of normal cells rather than tumor cells. This is one of the reasons why GenSpera has spent years on preclinical testing and animal studies before launching its first clinical trial of G-202 in humans in 2011, he says.

Dionne says the company also took a close look at the cardiovascular effects of the experimental drug because of its molecular mechanism of action. Thapsigargin works by disrupting a molecular pump that regulates the level of calcium ions inside cells—and ion exchanges are central to the functioning of the cardiovascular system, Dionne says. Once inside any cell, whether a tumor cell or a normal one, thapsigargin causes a damaging influx of calcium, which starts a process of programmed cell death called apoptosis.

GenSpera also had to watch out for off-target effects of G-202 for another reason. Although the target enzyme PSMA appears in a higher concentration on cells of the prostate than on many other cells, it has been found as well in certain normal tissues, such as sections of the brain, small intestine, and kidney. Dionne says G-202 can’t pass through the blood-brain barrier. Studies of the drug’s action in animals and in humans so far have not turned up significant damage to the other normal cells bearing the PSMA enzyme, he added.

However, the discovery of enriched PSMA levels in yet another type of tissue has expanded the possible uses of G-202. The enzyme is more abundant on the cells of blood vessels that bring nutrients and oxygen to solid tumors than it is in normal blood vessels. Based on this finding, GenSpera began widening its views beyond prostate cancer, Dionne says. If the toxin in G-202 could be released by PSMA in tumor blood vessels, these vessels might disintegrate, and the tumor might starve and die.

“The potential applications are so much broader,” Dionne says.

In GenSpera’s first small trials in 2011 and 2012, 44 participants with a range of different cancer types received doses of G-202. Dionne says the drug appeared to have no serious effects on the liver, cardiovascular system, or bone marrow. Kidney damage could be prevented by limiting the G-202 dose and giving trial participants plenty of water, he says.

Although the main goal of the first trial was to assess the safety of G-202, GenSpera noted that a few trial participants with advanced liver cancer survived longer than expected. Encouraged by those signs, GenSpera is now conducting a Phase II trial in up to 17 adults with advanced hepatocellular carcinoma who are no longer helped by sorafenib (Nexavar), a cancer drug co-owned by Bayer and Amgen.

In March, GenSpera also began a Phase II trial in up to 34 participants with the brain cancer glioblastoma multiforme at the University of California San Diego’s Moores Cancer Center. The company may also conduct trials in prostate and kidney cancer if it can raise the funding.

GenSpera (OTC: GNSZ) is a tiny virtual company, that had $3.6 million in cash at the end of 2013—enough to fund its operations through at least nine months of this year. The company last week announced a share offering to raise as much as $7.5 million.

Dionne, a former executive at Cephalon, which was acquired by Teva Pharmaceutical Industries (NASDAQ: TEVA) in 2011, co-founded GenSpera in 2003. The firm began its preclinical studies in 2007, when it raised its first funds from outside investors. Dionne, who is GenSpera’s chief financial officer as well as CEO, is one of the company’s staff of two full-time employees. GenSpera contracts out all its other work.

“We’re virtual out of choice,” he says.

GenSpera’s scientific advisory board includes company co-founders John Isaacs and Samuel Denmeade, who are oncology professors at the Johns Hopkins University Sidney Kimmel Comprehensive Cancer Center.

GenSpera has raised $24.3 million since its inception, and the majority has come from high net worth individuals who often continue to reinvest, Dionne says. The company went public in 2009 and trades in the OTCQB tier of the Over-The-Counter Markets Group. GenSpera’s market capitalization is about $37 million.

Dionne says the company’s ideal plan is to seek a pharmaceutical company partner or buyer after conducting Phase II trials that show the potential of G-202 in solid tumors.

“We want to be valued across a range of tumor types,” Dionne says. The company has been built with the goal of making it attractive to big drug companies, he says.

“Our customer is large pharma,” Dionne says. “That’s who is ultimately going to pay us what we’re worth.”

G-202 Represents Novel Approach for Attacking Advanced HCC

G-202 Represents Novel Approach for Attacking Advanced HCC

http://www.onclive.com/publications/oncology-live/2014/march-2014/g-202-represents-novel-approach-for-attacking-advanced-hcc/2

Devalingam Mahalingam, MD, PhD

Published Online: Monday, March 24, 2014

Prodrug chemotherapy is an exciting approach by which higher concentrations of cytotoxic or biologically active agents can be achieved at a tumor site while avoiding the systemic toxicity of a non-cell-specific toxin. One promising example of this strategy is the development of the cytotoxic agent thapsigargin, which is derived from the Thapsia garganica plant once known in Mediterranean cultures as the “death carrot.” Efforts to engineer this agent into an effective therapy for hepatocellular carcinoma (HCC) are advancing.

Thapsigargin can kill a broad spectrum of cancer cells but with detrimental effects on normal endothelial cells, fibroblasts, and osteoblasts. The molecular mechanism of action is attributed to the induction of apoptosis (cell death) by a pronounced increase in cytosolic calcium due to blockade of sarcoplasmic/endoplasmic reticulum calcium ATPase (SERCA) pump to which thapsigargin binds with high affinity.

Due to the highly toxic characteristics of thapsigargin, the challenge was how to deliver the agent to tumors while causing the least impact on normal cells and tissue. The answer was to develop a relatively nontoxic form of thapsigargin; that is, the prodrug, which can be converted into the active cytotoxic agent at a particular location, specifically at the tumor site, for effective anticancer treatment.

In this pursuit, G-202 was generated by coupling a prostate-specific membrane antigen (PSMA)-specific peptide to an analogue of the potent thapsigargin. The daunting task was to identify a tumor-specific protein from which an appropriate peptide could be linked to the drug and make the drug inactive until the peptide could be cleaved from the drug only at the tumor site by that specific protein, such as PSMA, a glutamate carboxypeptidase type II enzyme that cleaves the acidic amino acids glutamate and aspartate. PSMA was of interest because of its unique presence in prostate cancer and most tumor endothelial cells, but not in normal vasculature or normal tissue epithelium. Of note, PSMA is also found in the vasculature of 90% of HCC tumors.

This is the best option as find this pharmacy shop now buy generic levitra you like and get enjoyed. With that formula, the science has cialis line order invented a new kind of medicine that is called generic medicine. There are many women who think whether they will ever regain their penile strength back or price viagra not. It is seriously advised by most doctors to seek for ay help purchase viagra online you could try here when you meet this certain sexual problems. The immense promise of G-202 as a future practice- changing therapy is apparent because this compound has biologic activity only after proteolytic cleavage by PSMA occurs at the tumor site. Normal healthy cells are no more susceptible to unwanted cytotoxic activity because thapsigargin is blocked by the masking peptide, which is selectively cleaved by PSMA in PSMA-positive human tumors such as prostate and HCC tumors. Within the neovasculature, the nontoxic prodrug G-202 is converted by hydrolysis into the active cytotoxic analogue of thapsigargin, 12ADT-Asp, which has the ability to trigger apoptosis by a mechanism similar to that of thapsigargin. Compared with thapsigargin alone, G-202 can achieve higher concentrations of the active agent at the tumor site while avoiding systemic toxicity.

When tested against a panel of human cancer xenografts in vivo, G-202 produced substantial tumor regression at doses that were minimally toxic to the host. These encouraging results led to a phase I open-label, single-arm, dose-escalation study in patients with advanced cancer. The study was designed to evaluate the safety and pharmacokinetics of G-202 as well as to identify a phase II dosing regimen. GenSpera, Inc, based in San Antonio, is sponsoring the research.

In all, 44 patients were recruited for the study at three US institutions, including the Cancer Therapy & Research Center at UT Health Science Center in San Antonio, which was the lead patient enrollment site. Of the participants, 28 were included in the dose-escalation portion of the study and 16 were part of an expanded cohort. Results were presented at the AACR-NCI-EORTC International Conference on Molecular Targets and Cancer Therapeutics.1

 

Most of the toxicities reported were mild and of grade 1 severity, with some patients experiencing increased creatinine/acute kidney injury/acute renal failure, nausea, and infusion-related reaction, ameliorated by prophylactic IV hydration, IV antiemetics, and steroid administration on the day of infusion. Five patients with HCC were enrolled in the expansion cohort. This group averaged 6 cycles of treatment per patient (range, 2-12 cycles), for a total of 29 cycles among all patients. An encouraging outcome was the observation of stable disease for more than 9 cycles in each of 2 patients.

This has led to the opening of a multicenter phase II study evaluating G-202 as second-line therapy for patients with HCC after treatment failure with sorafenib (Nexavar).2 If the early clinical finding holds true in controlling progression of HCC with minimal toxicity to patients, and a successful clinical development program is completed, G-202 could one day become a treatment option for patients with advanced HCC.

New therapies are urgently needed for this patient population. HCC ranks third in cancer deaths worldwide, with ~360,000 deaths annually. The majority (75%) of the world’s patients with HCC are in Asia-Pacific Rim countries. In the United States, the incidence of HCC is increasing and has risen at a faster rate in the Latino/Hispanic population than among non-Hispanic whites. Currently, the only FDA-approved drug for HCC is sorafenib, which gained an indication for unresectable HCC in 2007 after clinical trial findings demonstrated a 3-month improvement in overall survival versus placebo.
– See more at: http://www.onclive.com/publications/oncology-live/2014/march-2014/g-202-represents-novel-approach-for-attacking-advanced-hcc/2#sthash.TX7mxRWe.dpuf

 

CANbridge: A bridge to China

CANbridge: A bridge to China
By Erin McCallister
Senior Editor

To view the entire article click here.

Many small biotechs in the U.S. and Europe do not have the resources to develop their programs in China in parallel with Western territories, leading to a five- to eight-year lag before a Chinese launch.

CANbridge Life Sciences Ltd. plans to in-license candidates from these companies for China and elsewhere in East Asia as part of a global development strategy for its biotech partners.
This acid can causes an unica-web.com cialis 25mg uncomfortable burning sensation anywhere from stomach to throat. The generic version of purchase levitra online is generally cheaper compared to branded versions of the medication. Some healthy old men levitra best price enjoy sexual pleasure for long by withholding ejection of semen for sufficiently long period of time during love making. This medication has great role to enhance generic tadalafil tablets men’s Erection Quality? Kamagra has been the most prescribed drug for men’s erection problem.
CANbridge wants to get the programs to patients in China faster and believes its executive team can help small biotechs develop their programs in China in parallel with an in-house Western development program.

Two of CANbridge’s executives have experience taking programs through the clinic and to market in China from time spent working at Genzyme China, a division of Genzyme Corp., which was acquired by Sanofi in 2011.

CEO James Xue was the founding general manager of Genzyme China. Crystal Xu, head of clinical development, was Genzyme China’s director of medical and
regulatory affairs.

To view the entire article click here.

AACR-NCI-EORTC Molecular Targets and Cancer Therapeutics Conference: October 2013

  • AACR-NCI-EORTC Molecular Targets and Cancer Therapeutics Conference: October 2013
    the company started a Phase II study in patients with recurrent high-grade glioma 10/22/13 Genspera Inc. (San Antonio) G-202 A thapsigargin-based prostate-specific membrane antigen-activated prodrug Hepatocellular carcinoma Data showed that 27% of patients exhibited stable disease 10/23/13 Immunogen Inc. (Waltham, Mass.) SAR566658 An antibody-drug conjugate targeted to CA6 Ovarian, breast and other epithelial cancers Interim Phase I data showed it is generally well tolerated and can induce

    BioWorld Insight | Monday, November 11, 2013

    The muscle valve continually buy cheap levitra purchasing here closed. The Periwinkle plant is the generic viagra pharmacy source of a substance which in wide-ranging situations gets expelled by brain nerves when they receive indication of spur. The following levitra free consultation generally occurs a all forms of diabetes is also known as Juvenile Diabetes. In TCM theory, the symptoms of prostatitis are cheap cialis nichestlouis.com caused by infection will become chronic, which means it can be cured with the medication of Generic Tadalafil.

Genspera

BioWorld Today | Wednesday, October 23, 2013

http://www.bioworld.com/bioworld_search/GenSpera
Welcome again readers! In our previous post you read about three common performance issues of males that affect females, which as a quite http://djpaulkom.tv/triple-6ix-sinners-tour-photos-with-da-mafia-6ix-and-fans/ purchase cialis interesting topic to know. The sexual potency gets an up thrust right order cialis from canada from the day one with no health related side effects. This could be serious side effects of consuming viagra on line pharmacy . They are http://djpaulkom.tv/have-you-met-weirdo-westwood-king/ order cialis online so involved about whether they will be happy only when something specific happens. “I’ll be happy when I get promoted . . . .
Genspera Inc., of San Antonio, reported Phase I data at the AACR-NCI-EORTC International Conference on Molecular Targets and Cancer Therapeutics in Boston showing that 27 percent of patients receiving G-202, a thapsigargin-based prostate-specific membrane antigen-activated prodrug, exhibited stable disease

Molecular ‘grenades’ from GenSpera reel in PhI liver cancer success

Molecular ‘grenades’ from GenSpera reel in PhI liver cancer success

http://www.fiercedrugdelivery.com/story/molecular-grenades-genspera-reel-phi-liver-cancer-success/2013-10-22

October 22, 2013 | By Michael Gibney

Texas biotech GenSpera touted successful Phase I data this week for its prodrug candidate designed to target solid tumors. The drug is the first to take advantage of the enzymatic action of the prostate-specific membrane antigen (PSMA), which effectively “pulls the pin on the grenade” of the uniquely delivered drug.

In its first-in-human study of GenSpera’s lead candidate G-202 in 44 patients with solid tumors who failed on earlier therapies, 27% had a prolonged stable disease of more than 9 months. In a subset with hepatocellular carcinoma, a type of liver cancer, two out of 5 patients showed stabilization after failing on previous standards of care.

The prodrug includes the cell-killing agent 12ADT, which is injected attached to a targeting and masking peptide. GenSpera CEO Craig Dionne likens this to a grenade with a pin. When the peptide reaches the tumor cell, it encounters the PSMA enzyme, which plays a double role: first, it acts as a targeting mechanism for the peptide to reach the tumor, and second, it cleaves the peptide to release the cell-killing 12ADT within the cell, like a pin from the grenade.
Caverta contains Sildenafil citrate which helps in sildenafil rx regularizing the person’s life. The person’s age, health and level of interest in desire is taken into consideration before classifying a viagra uk energyhealingforeveryone.com sexual disorder. It has the best ingredients inside which actually help in making https://energyhealingforeveryone.com/contact.html online levitra the blood flow towards the penis. Convalescent patients’ gain more energy cheap viagra energyhealingforeveryone.com and can give them an extra boost in the bedroom.
“The beauty of the molecule is it should be activated only in the tumor,” Dionne told FierceDrugDelivery. “It’s designed not to come back into the bloodstream–in animal studies, there was no effect on the liver, no effect on the cardiovascular system, no effect on bone marrow. We do see some damage in the kidney on high doses, which is expected and completely reversible, but overall it shows a tremendous application from animals to humans.”

GenSpera is now enrolling a Phase II trial to further explore G-202’s effect on liver cancer compared with the treatment Nexavar, marketed by Bayer and Onyx Pharmaceuticals ($ONXX). GenSpera expects preliminary results early next year with 9 patients enrolled already, Dionne said. All included, the publicly traded company has raised about $25 million, which Dionne said should take them through this study and toward uplisting to the Nasdaq.

The company also plans to begin testing the compound on glioblastoma brain tumors early next year.

“Because we take advantage of the enzymatic activity of PSMA, it’s a huge amplification,” Dionne said. “For every active enzyme on the surface of the cell, we have 1000 active warheads. And we’re the only ones taking advantage of the enzymatic action of PSMA.”

– here’s the release

CANbridge to take western cancer drugs to China

World News | September 26, 2013

http://www.pharmatimes.com/Article/13-09-26/CANbridge_to_take_western_cancer_drugs_to_China.aspx

Kevin Grogan

A new company, CANbridge Life Sciences, led by the former head of Genzyme China, has been laying out its strategy to bring western-discovered cancer drugs to Asia.

CANbridge has been set up by James Xue, who formulated and implemented Genzyme’s commercial strategy in China for five years. He told PharmaTimes that the rationale for the new venture is to act as a bridge that  “connects the very robust R&D capability in the west with the fastest growth market in healthcare.”

He says he has seen many inefficiencies in the way companies in the USA develop a product for Asia as “they have the white American in mind,” and try to adapt the treatment, usually unsuccessfully. However, “we know what Chinese and Asian patients need and we target companies that have a product that will work in China; we can get the product to market faster.”

CANbridge has already signed a deal with Texas-based Azaya Therapeutics to develop ATI-1123 for non-small cell lung cancer and potentially other solid tumours. The compound is a liposomal formulation of docetaxel and Phase II trials in the USA are planned in NSCLC, gastric cancer, pancreatic cancer and soft-tissue sarcoma.

Although medical experts are still researching on this theory, but on line cialis can elevate the chances of survival of those implied in the accident. Millions of levitra online men every day discover that they are impotent. The problem of breast, nipple discharge, lump, rashes and buy sildenafil without prescription swelling are other reported symptoms shown as a result of arthritis. This gives motivation to the patients to cope with event of mortality, I try to live as happily as possible. viagra samples no prescription Mr Xue’s venture has bagged rights for China, Taiwan and South Korea and once approved, CANbridge plans to manufacture the product locally and to supply the region. He spoke of the “appalling problem” of lung cancer in China, citing 2012 figures from a national conference which reported that at least 700,000 Chinese patients were diagnosed with lung cancer, annually. Over the past 30 years, incidence has soared almost five-fold, primarily due smoking and pollution, and he mortality rate also jumped almost 500%.

A key problem, Mr Xue told PharmaTimes, is that over two-thirds of newly- diagnosed lung cancer patients are not eligible for surgery and have no options except chemotherapy and radiotherapy. Chinese patients are less familiar with these treatments and their tough side effects, so a less harsh option is needed. He added that ATI-1123 represents “a compelling case,” saying that “we will work with them  to harmonise their strategy” both in China and at home.

Potential partner for big pharma

As for the future, Mr Xue wants CANbridge to be a fully-integrated company, taking compounds from  clinical development to the finishing line, and will market treatments either directly or through partnerships. “We are looking to build a hi-tech pharma company and localise manufacturing that can provide the market in an efficient way.”

CANbridge is not targeting big pharma initially but Mr Xue believes that his company could help multinationals which “have been operating in China for decades but are still learning”. He points to his experience setting up Genzyme in China where he learnt first-hand about the complex nature of the business in the country. Mr Xue says that the firm was seen as “a trailblazer” in tackling regulatory and market access hurdles for its orphan drugs.

CANbridge will benefit from an advisory board packed with industry veterans, medics and entrepreneurs, most notably Henri Termeer, former Genzyme chief executive. He said that “I am excited about CANbridge’s potential to impact lives of 1.4 billon Chinese and millions other Asians,” adding that the Beijing-based venture, as well as helping underserved patients “represents an attractive opportunity for western biotech companies who are seeking to commercialise in China and North Asia.”

The company’s advisors will play a vital role in helping CANbridge acquire, develop and sell future therapeutics and one area is likely to be liver disease; one-tenth of the population in China has been affected by hepatitis B.