Last update 21 Nov 2024

Valrubicin

Last update 21 Nov 2024

Overview

R&D Status

Clinical Result

Translational Medicine

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

(8S, 10S)-8-glycoloyl-7,8,9,10-tetrahydro-6,8,11-trihydroxy-1-methoxy-10-[[2,3,6-trideoxy-3-(2,2,2-trifluoroacetamido)-α-L-lyxo-hexopyranosyl]oxy]-5,12-naphthacenedione 8²-valerate, 2-oxo-2-[(2S,4S)-2,5,12-trihydroxy-7-methoxy-6,11-dioxo-4-({2,3,6-trideoxy-3-[(trifluoroacetyl)amino]hexopyranosyl}oxy)-1,2,3,4,6,11-hexahydrotetracen-2-yl]ethyl pentanoate, N-Trifluoroacetyladriamycin-14-valerate

+ [7]

Target

Top II

Mechanism

Top II inhibitors(Topoisomerase II inhibitors)

Therapeutic Areas

NeoplasmsUrogenital Diseases

Active Indication

Carcinoma in situ of bladder

Inactive Indication

Carcinoma in SituNon-Muscle Invasive Bladder NeoplasmsOvarian Cancer+ [5]

Originator Organization

Endo International Plc

Active Organization

Endo Operations Ltd.

Inactive Organization

Anthra Pharmaceuticals, Inc.Endo Pharmaceuticals, Inc.Bayer Schering Pharma AG

+ [1]

Drug Highest PhaseApproved

First Approval Date

US (25 Sep 1998),

Carcinoma in situ of bladder

RegulationOrphan Drug (US)

Structure

Molecular FormulaC34H36F3NO13

InChIKeyZOCKGBMQLCSHFP-KQRAQHLDSA-N

CAS Registry56124-62-0

Clinical Trials associated with Valrubicin

NCT01606345 / CompletedPhase 1IIT

Phase I Dose Escalation and Landmark Study of Percutaneous Valrubicin for Upper Tract Urothelial Carcinoma (UTUC) Following Endoscopic Resection

The purpose of this study is to learn more about how well the drug valrubicin (VALSTAR®) works to help treat the patient's cancer when administered through a nephrostomy tube inserted through their back into their kidney. The study is also being done to determine how safe and easy it is to tolerate valrubicin at specific dose levels, as well as the way in which the drug is eliminated from the human body (Pharmacokinetics or PK).

Start Date01 Jul 2012

Sponsor / Collaborator

H. Lee Moffitt Cancer Center & Research Institute, Inc.

[+1]

NCT01310803 / TerminatedPhase 3

A PHASE 3B, RANDOMIZED, OPEN-LABEL, MULTI-CENTER STUDY TO EVALUATE THE EFFICACY AND SAFETY OF MAINTENANCE THERAPY WITH VALRUBICIN VERSUS NO MAINTENANCE, IN SUBJECTS TREATED WITH VALRUBICIN INDUCTION FOR CARCINOMA IN SITU (CIS) OF THE BLADDER

This is a Phase 3b open-label, randomized, parallel-arm, multicenter study to evaluate the efficacy and safety of 10 monthly intravesical administrations of maintenance therapy with valrubicin following induction with valrubicin as compared to induction with valrubicin only in subjects with CIS of the bladder. The randomization will be 1:1 and subjects will be stratified by tumor type (CIS plus papillary disease vs. CIS only) and time from last bacillus Calmette-Guerin (BCG) failure (>1 year vs. <1 year).

Start Date01 May 2011

Sponsor / Collaborator

Endo Pharmaceuticals, Inc.

EUCTR2010-023789-33-DE / Not yet recruitingNot Applicable

A phase IIa, multicenter, randomized, two-arm, observer-blind, vehicle and reference controlled proof of concept trial to investigate intra-individually (left/ right) the antipsoriatic efficacy and safety of once daily topical application of Valrubicin cream 1 % in comparison to vehicle and reference product in adult patients with stable plaque psoriasis

Start Date17 Feb 2011

Sponsor / Collaborator

Valderm ApS

100 Clinical Results associated with Valrubicin

100 Translational Medicine associated with Valrubicin

100 Patents (Medical) associated with Valrubicin

162

Literatures (Medical) associated with Valrubicin

01 Oct 2024·Anticancer Research

Repurposing Valrubicin as a Potent Inhibitor of Ovarian Cancer Cell Growth

Article

Author: LEE, JAEEUN ; HEO, KYUN ; Lee, Jaeeun ; Heo, Kyun

BACKGROUND/AIMOvarian cancer (OC) is a leading cause of cancer-related mortality among women, and there remains a significant unmet need for new therapeutic agents to improve patient outcomes. This study aimed to explore drug repositioning by screening a library of Food and Drug Administration (FDA)-approved compounds to identify those with therapeutic potential against OC. We also aimed to elucidate the molecular mechanisms of action of such compounds to better understand how they inhibit cancer cell proliferation.MATERIALS AND METHODSUsing the WST-1 assay, a library of 1710 FDA-approved drugs was screened to evaluate their effects on OC cell proliferation. The molecular mechanisms underlying the effects of selected compounds were assessed through terminal deoxynucleotidyl transferase-mediated dUTP nick end labeling (TUNEL) assay and immunoblot analysis.RESULTSScreening of FDA-approved libraries revealed valrubicin as a potent inhibitor of OVCAR8 cell proliferation and SKOV3 and A2780 cell growth. Furthermore, valrubicin treatment led to increased DNA fragmentation, as evidenced by the TUNEL assay, and activated apoptosis signaling through enhancement of cleaved caspase-3 and poly(ADP-ribose) polymerase levels.CONCLUSIONValrubicin, through drug repositioning, can be applied as a new therapeutic agent for OC.

01 Sep 2024·Urologic Oncology: Seminars and Original Investigations

Early experience with sequential intravesical gemcitabine and docetaxel for micropapillary variant non-muscle invasive bladder cancer

Article

Author: McElree, Ian M ; O'Donnell, Michael A ; Packiam, Vignesh T ; Mott, Sarah L ; Abou Chakra, Mohamad

BACKGROUNDGuidelines lack clear recommendations regarding conservative management of micropapillary (MP) variant non-muscle invasive bladder cancer (NMIBC). Bladder-sparing therapy using intravesical Bacillus Calmette-Guerin (BCG) has been reported although there are concerns regarding recurrence and progression with this approach. Due to the ongoing BCG shortage, we have utilized sequential intravesical gemcitabine and docetaxel (Gem/Doce) as primary therapy for NMIBC, including some cases with limited MP urothelial carcinoma (MPUC). To compare oncologic outcomes of patients with non-muscle invasive MPUC and conventional UC treated with Gem/Doce.METHODSA secondary analysis of 138 patients with high-risk NMIBC treated with intravesical Gem/Doce from January 2011 to December 2021 was performed. Oncologic outcomes were compared in patients with or without MPUC using the Kaplan-Meier method.RESULTSMedian follow-up (f/u) for all patients was 23 months (IQR 13-34). There were 129 patients with pure UC and 9 with MPUC. In those with MPUC, all were high-grade (HG), 8/9 were stage T1, 7/9 had a focal MP component (extent < 10%), 3/9 had concomitant CIS, and 2/9 had lymphovascular invasion. All MPUC tumors were re-resected, and 4 had T0, 3 had T1 HG, 1 had Ta HG, 1 had carcinoma in situ (CIS); none had residual MP or LVI tumors before Gem/Doce treatment. The 24-month high-grade recurrence-free survival was 89% and 80% in patients with MPUC and pure UC, respectively. Survival outcomes did not significantly differ between patients with and without MPUC. Four patients with MPUC experienced recurrent NMIBC after Gem/Doce, and all were treated successfully with rescue sequential intravesical valrubicin and docetaxel (Val/Doce). Pathology of these four recurrent patients revealed more aggressive histologic features in the original tumor including: multifocal tumor (3/4), T1 HG disease (4/4), concomitant CIS (2/4), and moderate MP variant extent (30%) (1/4). No patient with MPUC underwent cystectomy, experienced progression, or died at last follow-up (median f/u of 43 months).CONCLUSIONSGem/Doce with Val/Doce rescue appears to have activity against carefully selected non-muscle invasive MPUC with favorable histology. Larger prospective trials are needed to validate these results.

01 Sep 2024·Expert Opinion on Drug Safety

Comparative analysis of adverse events among intravesical drugs in bladder cancer: a real-world study on FAERS database

Article

Author: Xu, Tao ; Qin, Caipeng ; Peng, Yun ; Du, Yiqing ; Song, Yuxuan

BACKGROUNDIntravesical therapy is a commonly utilized treatment for non-muscle invasive bladder cancer (NMIBC). This study focuses on summarizing the signals of all intravesical drugs and aims to highlight the comprehensive differences in adverse events (AEs) between these drugs.RESEARCH DESIGN AND METHODSWe conducted pharmacovigilance data analysis based on the real-world big data from the Food and Drug Administration Adverse Event Reporting System (FAERS) database.RESULTSWe elucidated all signals compared with the overall FAERS database or other administration routes for Bacillus Calmette-Guerin (BCG), mitomycin, gemcitabine, valrubicin, and epirubicin. Notably, the distribution of reported AEs associated with intravesical therapy exhibited a noticeable inclination toward male patients. Furthermore, all five drugs demonstrated a disproportionate distribution in local AEs, particularly in renal and urinary disorders. Additionally, specific signals and findings were summarized for each individual drug. Finally, we highlighted the AEs that resulted in serious outcomes for each drug.CONCLUSIONWe have compiled an overview of the AEs tied to intravesical drugs whilst considering their individual distinctions. These insightful findings serve to enrich our comprehension of the safety profiles and potential risks linked to intravesical therapy.

News (Medical) associated with Valrubicin

05 Feb 2024

·www.biospace.com

ImmunityBio Quality-of-Life Study in BCG-Unresponsive Bladder Cancer Trial Indicates Improved Physical Function in the 71% Complete Responders Suggesting a Favorable Risk-Benefit Ratio for N-803 Plus BCG

Patient Reported Outcomes (PROs) based on a May 16, 2022 data cutoff in the QUILT 3.032 trial indicate stability of physical function and global health in patients who completed PRO questionnaires and reached month 24 on-study Overall, participants with complete responses (CRs) to combination therapy with the novel interleukin-15 (IL-15) superagonist N-803 and bacillus Calmette-Guerin (BCG) reported better physical function than those who did not achieve a CR at month 6 Stability of these PROs supports the safety and tolerability of the potential new treatment combination Taken together with the positive durable 71% response and 89.2% cystectomy avoidance rates in cohort A and a favorable safety pro the May 16, 2022 data cutoff, along with the available PROs, support a favorable risk-benefit ratio for N-803 plus BCG in this patient population The Food and Drug Administration (FDA) is currently reviewing the Biologics License Application (BLA) for N-803 plus BCG for the treatment of NMIBC CIS with a Prescription Drug User Fee Act (PDUFA) date of April 23, 2024 CULVER CITY, Calif.--(BUSINESS WIRE)-- ImmunityBio, Inc. (NASDAQ: IBRX), a clinical-stage immunotherapy company, today announced that findings from Patient-Reported Outcomes (PROs) of participants in the phase 2/3 QUILT 3.032 study of N-803 plus BCG in BCG-unresponsive non-muscle invasive bladder cancer (NMIBC) were published by the peer-reviewed journal Urology Practice. These PROs support the positive interim results from the study published in NEJM Evidence, wherein 71% of patients in cohort A with CIS with or without Ta/T1 disease achieved a complete response. The published PROs based on a May 16, 2022 data cutoff indicate that both physical function and global health as self-reported by QUILT 3.032 participants with BCG-unresponsive NMIBC CIS (cohort A) or papillary disease (cohort B), remained stable over the 2-year course of the study for patients who completed the PRO questionnaires and reached 24 months on-study. In addition, overall both cohort A and B participants who reached month 24 on-study and also completed an NMIBC-specific questionnaire focusing on the challenges of bladder cancer, also reported no decline of their health or urinary tract-related symptoms while in the study. Overall, participants who achieved a complete response with the novel combination therapy reported better physical function by month six of the study than those who did not achieve a complete response. “The self-reported stability of health and physical function over the course of the study by the participants reflect another aspect of safety and tolerability of this new combination therapy,” said Patrick Soon-Shiong, M.D., Executive Chairman and Global Chief Scientific and Medical Officer at ImmunityBio. “Taken together with the positive response rate in cohort A of over 70%, the persistence of responses and cystectomy avoidance, these QoL findings suggest a favorable risk-benefit ratio for this potential new therapeutic option for patients with BCG-unresponsive bladder cancer.” The finding of relative stability of global health and physical function during the course of the study is similar to that reported by others for BCG monotherapy, suggesting the novel combination is as tolerable as treatment with BCG alone. “Many current therapies for bladder cancer slow disease progression but can cause debilitating side effects,” said Principal Investigator Karim Chamie, M.D., Associate Professor of Urology at UCLA. “The data from the QUILT 3.032 Quality of Life study suggest that many patients not only have a durable response but also report no decline in physical function, which is very important for these patients.” QUILT 3.032 Study Details The ongoing phase 2/3 open-label multicenter registrational study QUILT 3.032 (NCT03022825) is evaluating the safety and efficacy of the investigational interleukin-15 superagonist N-803 (also known as Anktiva® and nogapendekin alfa inbakicept, NAI) in combination with a standard therapy for NMIBC, bacillus Calmette-Guerin (BCG), in patients who failed or in whom cancer returned after BCG monotherapy, and thus were diagnosed as BCG-unresponsive. The study comprises three cohorts, with cohort A enrolling patients with carcinoma in situ (CIS) with or without Ta/T1 disease and cohort B enrolling patients with high grade Ta/T1 papillary disease. Both cohorts A and B received combination N-803 plus BCG therapy. Cohort C patients, with CIS +/- Ta/T1 disease received N-803 monotherapy. The primary end point is the incidence of CR at the 3- or 6-month assessment visit for cohorts A and C, and the disease-free survival (DFS) rate at 12 months for cohort B. Durability, cystectomy avoidance, progression-free survival, disease-specific survival (DSS), and overall survival are secondary end points for cohort A. Cohort C was discontinued due to a low response rate with N-803 monotherapy, per study design. The FDA has accepted for review ImmunityBio’s resubmission of its biologics license application (BLA) for N-803 plus BCG for the treatment of BCG-unresponsive NMIBC CIS with or without Ta or T1 disease, and has set a user fee goal date (PDUFA date) of April 23, 2024. Bladder cancer is the 10th most-commonly diagnosed cancer, with approximately 80% of newly diagnosed cases being NMIBC. Intravesical (directly to the bladder) instillation of BCG after removal of cancer tissue from the lining of the bladder (transurethral resection of the bladder tumor; TURBT) is Standard-of-Care (SoC) for intermediate and high-risk NMIBC patients, but up to 40% of patients will fail BCG therapy and ~50% will relapse after an initial response and given a diagnosis of being BCG-unresponsive. Therapies approved by the FDA for this indication include pembrolizumab, nadofaragene, combined gemcitabine and docetaxel, and valrubicin. Radical cystectomy – surgical removal of the bladder - is also an option for these patients. QUILT 3.032 is being conducted to address the need for a safe, effective therapeutic option for BCG-unresponsive NMIBC patients that provides an opportunity for avoidance of radical cystectomy. N-803 is investigational. Safety and efficacy have not been established by any Health Authority or Agency, including the FDA. About ImmunityBio ImmunityBio is a vertically-integrated, clinical-stage biotechnology company developing next-generation therapies and vaccines that bolster the natural immune system to defeat cancers and infectious diseases. The Company’s range of immunotherapy and cell therapy platforms, alone and together, act to drive and sustain an immune response with the goal of creating durable and safe protection against disease. ImmunityBio is applying its science and platforms to treating cancers, including the development of potential cancer vaccines, as well as developing immunotherapies and cell therapies that ImmunityBio believes sharply reduce or eliminates the need for standard high-dose chemotherapy. These platforms and their associated product candidates are designed to be more effective, accessible, and easily administered than current standards of care in oncology and infectious diseases. For more information, please visit Immunitybio.com. Forward Looking Statements This press release contains forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995, such as statements regarding data and results from ongoing clinical trials and potential implications therefrom, potential benefits to patients, potential treatment outcomes for patients, the regulatory review process and timing thereof, market and prevalence data, and ImmunityBio’s investigational agents as compared to other existing and potential treatment options, among others. While ImmunityBio believes the BLA resubmission addresses the issues identified in the FDA’s complete response letter, there is no guarantee that the FDA will ultimately agree that such issues have been successfully addressed and resolved. Statements in this press release that are not statements of historical fact are considered forward-looking statements, which are usually identified by the use of words such as “anticipates,” “believes,” “continues,” “goal,” “could,” “estimates,” “scheduled,” “expects,” “intends,” “may,” “plans,” “potential,” “predicts,” “indicate,” “projects,” “seeks,” “should,” “will,” “strategy,” and variations of such words or similar expressions. Statements of past performance, efforts, or results of our preclinical and clinical trials, about which inferences or assumptions may be made, can also be forward-looking statements and are not indicative of future performance or results. Forward-looking statements are neither forecasts, promises nor guarantees, and are based on the current beliefs of ImmunityBio’s management as well as assumptions made by and information currently available to ImmunityBio. Such information may be limited or incomplete, and ImmunityBio’s statements should not be read to indicate that it has conducted a thorough inquiry into, or review of, all potentially available relevant information. Such statements reflect the current views of ImmunityBio with respect to future events and are subject to known and unknown risks, including business, regulatory, economic and competitive risks, uncertainties, contingencies and assumptions about ImmunityBio, including, without limitation, (i) the risks and uncertainties associated with the regulatory review process, (ii) whether or not the FDA will ultimately determine that the BLA resubmission and related actions successfully addresses and resolves the issues identified in the FDA’s complete response letter, (iii) uncertainties regarding the timeline of FDA review of the resubmitted BLA, (iv) any inability to successfully work with the FDA to find a satisfactory solution to address any concerns in a timely manner or at all during the review process for the BLA, including any inability to provide the FDA with data, analysis or other information sufficient to support an approval of the BLA, (v) the ability of ImmunityBio and its third party contract manufacturing organizations to adequately address the issues raised in the CRL, (vi) any potential facility re-inspections that may be required regarding ImmunityBio’s third party contract manufacturing organizations or otherwise and results therefrom, (vii) whether the FDA accepts the data and results as included in the BLA resubmission at levels consistent with the published results, or at all, (viii) the ability of ImmunityBio to continue its planned preclinical and clinical development of its development programs through itself and/or its investigators, and the timing and success of any such continued preclinical and clinical development and planned regulatory submissions, (xi) ImmunityBio’s ability to retain and hire key personnel, (ix) ImmunityBio’s ability to obtain additional financing to fund its operations and complete the development and commercialization of its various product candidates, (x) ImmunityBio’s ability to successfully commercialize its product candidates and uncertainties around regulatory reviews and approvals, (xi) ImmunityBio’s ability to scale its manufacturing and commercial supply operations for its product candidates and future approved products, and (xii) ImmunityBio’s ability to obtain, maintain, protect and enforce patent protection and other proprietary rights for its product candidates and technologies. More details about these and other risks that may impact ImmunityBio’s business are described under the heading “Risk Factors” in the Company’s Form 10-K filed with the U.S. Securities and Exchange Commission (“SEC”) on March 1, 2023 and the Company’s Form 10-Q filed with the SEC on November 9, 2023, and in subsequent filings made by ImmunityBio with the SEC, which are available on the SEC’s website at . ImmunityBio cautions you not to place undue reliance on any forward-looking statements, which speak only as of the date hereof. ImmunityBio does not undertake any duty to update any forward-looking statement or other information in this press release, except to the extent required by law.

Clinical ResultImmunotherapy

15 Jun 2022

·www.biospace.com

ImmunityBio’s Patrick Soon-Shiong Discusses Quest to Orchestrate NK and T Cells

Dr. Patrick Soon-Shiong, M.D./Courtesy of ImmunityBio Three decades after first writing about how natural killer cells (NK) functioned, Dr. Patrick Soon-Shiong, M.D., and his company, ImmunityBio, Inc. are on the final leg of what they hope will be U.S. Food and Drug Administration approval of their drug, N-803 (anktiva), for the treatment of bladder cancer. In the late 1980s, Soon-Shiong was a professor and surgeon at the UCLA School of Medicine specializing in pancreatic cancer and transplants of the organ. But he had a dilemma dealing with the body’s immune system that both hindered and helped what he was trying to accomplish. NK cells were responsible for causing organ rejection while those same cells killed the cancer in the pancreas. Continuing on the earlier efforts of Dr. Anthony M. Sun, M.D. of Connaught Laboratories in Toronto, who was experimenting on rats to reverse diabetes, Soon-Shiong enhanced Sun’s encapsulation method for islets made from a gel that came from seaweed. He devised a purified formula that improved how islets pass insulin, glucagon, oxygen and hormones while blocking antibodies and T cells in the immune system which would otherwise destroy the islets. “I’ve been pursuing that for the rest of my career, trying to figure out how to orchestrate NK cells and T cells,” Soon-Shiong told BioSpace. What followed was Soon-Shiong performing the world’s first encapsulated human islet transplant, the first engineered islet cell transplant and the first pig to man islet cell transplant in a diabetic patient. Besides trying to orchestrate cells, Soon-Shiong was also choreographing business deals to advance his research. His business acumen generated the revenue that led to his most successful medical achievement to date, Abraxane (paclitaxel), which is helping to finance his future endeavors, including anktiva. But it hasn't been without family turmoil. In 1991, along with his brother, Soon-Shiong co-founded VivoRx, which was followed by a second startup called VivoRx Pharmaceuticals. A legal fight between the brothers forced Soon-Shiong out of VivoRX. He left with VivoRx Pharmaceuticals and changed its name to American Bioscience. Soon-Shiong also founded a second company called American Pharmaceutical Partners and acquired two money-losing factories for it. He was soon able to turn those businesses into money makers. Soon-Shiong used the income for research and development into improving the generic chemotherapy drug paclitaxel. He called his re-worked version of paclitaxel Abraxane, and it performed better in clinical trials and was less likely to cause allergic reactions. Abraxane is an albumin-bound form of paclitaxel, now indicated for the treatment of breast cancer, non-small cell lung cancer, pancreatic cancer, ovarian cancer, cancer of the fallopian tubes and primary peritoneal cancer. In 2005, the FDA approved Abraxane and American Pharmaceutical shares jumped 47%. A short time after the FDA’s decision, Soon-Shiong announced he would combine his publicly traded American Pharmaceutical with privately held American BioScience, of which he owned 80%. To do this, American Pharmaceutical would issue 86 million new shares to American BioSience. The wheeling and dealing added about $2.5 billion to Soon-Shiong’s wealth while smaller investors questioned the ethics of the transaction. Fifteen months after merging the companies, Soon-Shiong split them into two new businesses, APP Pharmaceuticals and Abraxis, which held the rights to Abraxane. In 2008 and 2010 Soon-Shiong sold his two companies for a total of $9.1 billion. The poor kid from South Africa had obtained the American dream. Besides his work in the life sciences industry, the eclectic Soon-Shiong has used his wealth for some of his other interests. A self-proclaimed news junkie, he bought the Los Angeles Times and San Diego Union-Tribune. As a big fan of basketball, he purchased a minority position in the Los Angeles Lakers by taking over the ownership stake of team legend Ervin “Magic” Johnson and got courtside seats for their games. But medical science is Soon-Shiong’s primary focus, which brings us to the here and now. Soon-Shiong’s clinical-stage immunotherapy company, ImmunityBio, which he founded in 2014, had already received Breakthrough Therapy and Fast Track designations from the FDA for N-803, when in May the company submitted a Biologics License Application. N-803 is a first-in-class IL-15 superagonist, plus Bacillus Calmette-Guérin (BCG) intended for the treatment of BCG-unresponsive non-muscle invasive bladder cancer (NMIBC) carcinoma in situ (CIS) with or without Ta or T1 disease. If N-803 receives approval, it will be the first FDA-approved immunotherapy since BCG in 1990 that can be delivered directly to the bladder to induce natural killer cells and T cells. It will also be the Culver City, California company’s first FDA-sanctioned product. “It’s one of the first opportunities to show that N-803 actually activates and proliferates NK cells and T cells and drives memory T cells for your innate immune system to treat cancer and infectious diseases,” Soon-Shiong, who turns 70 in July, said. What are the challenges in developing N-803? “It’s a biologic,” Soon-Shiong said. “It's really a paradigm shift in the sense that we want to preserve your immune system. So, the challenge is, how do we break the 40-year current standard of care where we give high-dose chemotherapy and high-dose radiation, which counterintuitively wipes out your NK cells and T cells. So, we needed to find ways to address this and in 2017, I'm pleased to say that the Oncology Center of Excellence under (director) Dr. (Richard) Pazdur, gave us the opportunity to launch this under the QUILT trial program.” The goal of N-803 is to reduce the chances a patient will need surgery and its tremendous cost. “Patients who are BCG unresponsive face the surgical procedure called radical cystectomy,” Soon-Shiong said. “Unfortunately, it’s fraught with a 9% mortality, a 60% morbidity, high cost, terrible quality of life, losing a bladder in elderly patients, nephritis infection, visits to the hospital, and it’s one of the costliest procedures in healthcare for cancer. So, there was a great unmet need of avoiding radical cystectomy and we followed that [FDA] guidance in the trial design.” The BLA submission for BCG-unresponsive NMIBC is based on data from 171 subjects from Phase I and II trials in bladder cancer and 84 subjects treated in ImmunityBio’s Pivotal Phase II/III QUILT 3032 study of the combination of N-803 and BCG. There was a 71% complete remission rate according to the study’s data. Patients who had failed on previous therapies showed an over 50% increase in both response and median duration compared to the FDA-approved alternatives, Endo’s Valstar (valrubicin) and Merkc's Keytruda (pembrolizumab), a systemic checkpoint inhibitor therapy for this indication. “You could see a 26.6-months median duration of response and significant reduction of cystectomy with a very, very tolerable profile. [It] validates this hypothesis by harnessing the natural killer cells and T cells. You can get durable memory,” Soon-Shiong said. Data presented from the QUILT 3032 study by the company at the American Society of Oncology’s annual meeting also showed that at 24 months there was a 96% avoidance of bladder cancer progression, patients had a cystectomy avoidance rate of 91% and there was 100% overall survival for bladder cancer in responders. Additionally, N-803 showed promise in treating pancreatic cancer. In a Phase II QUILT 88 clinical trial, patients with advanced pancreatic cancer who were treated with the Nant Cancer Vaccine, N-803 and off-the-shelf PDL1-targeted high-affinity NK cell infusion showed more than double the median overall survival rate compared to historical survival data. Median overall survival for patients with third- to sixth-line pancreatic cancer was 6.2 months. Soon-Shiong holds over 200 patents and ImmunityBio is currently working on 27 clinical trials. To keep the research going, Soon-Shiong is spending his own money to support those projects. “I've personally made a significant investment and I'll continue to do so. We need to, but I'm confident that the data and the results will generate the appropriate resources needed for us to pursue what we’re doing,” Soon-Shiong said. One group that needs convincing that ImmunityBio is on the right track is Wall Street. The company’s stock has dropped about 90% over the past 14 months. But Soon-Shiong isn’t concerned. “Wall Street follows rather than leads and we need to lead,” he said. “We do care about the shareholders, but what we need to do is generate organic value. Abraxane was proof of that when we were developing a vaccine and went public in 2001. “If you go back and look at the history of American Pharmaceutical Partners, it followed the exact same strategy where the stock fell down to single digits and nobody would believe this drug would get approved and it's now at a billion dollars in sales. So, I think you just have to have complete belief in the science, which we do, and the validity of each application.” Soon-Shiong’s work on N-803 could have additional benefits, like fighting COVID-19. In 2020, he was selected by the federal government to participate in “Operation Warp Speed,” which was established to accelerate the development of vaccines. “I've said since 2020 when COVID broke out that unless we generated a vaccine that is not just antibody-based but T cell and NK cell-based, we will never stop transmission. More importantly, an antibody-based vaccine will actually enhance the mutational evolution of this virus and create what we now see facing us today," Soon-Shiong said. If anktiva is approved by the FDA, what will it mean personally for Soon-Shiong? “This would be the first validation, all the way to the FDA if it were approved, that indeed, you do not need chemotherapy,” he said. “If you can take a patient's own immune system and activate it, you can get a complete remission.” A final decision by the FDA on N-803 is expected in 2023.

AntibodyBreakthrough TherapyFirst in ClassVaccineImmunotherapy

100 Deals associated with Valrubicin

External Link

KEGG	Wiki	ATC	Drug Bank
D02697	Valrubicin	L01DB09	DB00385

R&D Status

Approved

10 top approved records.

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Indication	Country/Location	Organization	Date
Carcinoma in situ of bladder	US	Endo Operations Ltd.	25 Sep 1998

Developing

10 top R&D records.

to view more data

Indication	Highest Phase	Country/Location	Organization	Date
Renal Pelvis and Ureter Urothelial Carcinoma	Discovery	US	Endo Pharmaceuticals, Inc.	01 Jul 2012
Carcinoma in Situ	Discovery	US	Endo Pharmaceuticals, Inc.	01 May 2011
Carcinoma in situ of bladder	Discovery	US	Endo Pharmaceuticals, Inc.	01 May 2011
Non-Muscle Invasive Bladder Neoplasms	Discovery	US	Endo Pharmaceuticals, Inc.	01 May 2011
Non-Muscle Invasive Bladder Neoplasms	Discovery	US	Endo Pharmaceuticals, Inc.	01 May 2011
Transitional Cell Carcinoma	Discovery	US	Endo Pharmaceuticals, Inc.	01 May 2011
Recurrent Bladder Cancer	Discovery	US	Anthra Pharmaceuticals, Inc.	01 Dec 1996
Recurrent Bladder Cancer	Discovery	CA	Anthra Pharmaceuticals, Inc.	01 Dec 1996
Ovarian Cancer	Discovery	US	Anthra Pharmaceuticals, Inc.	15 Nov 1995
Ovarian Cancer	Discovery	US	Bayer Schering Pharma AG	15 Nov 1995

Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


AUA2022	Not Applicable	Non-Muscle Invasive Bladder Neoplasms	-	Valrubicin and Docetaxel	qbukskdafp(qziejsspgo) = 24% jamzurvsvv (ouuxsqovwa ) View more	-	01 May 2022
ASCO_GU2022	Not Applicable	Carcinoma of urinary bladder, invasive	75	Valrubicin-DocetaxelValrubicin-Docetaxel	(sisawbigbk) = 24% npmnclojcc (vxkytmkytx ) View more	Positive	16 Feb 2022
NCT01310803 (CTgov)	Phase 3	Carcinoma in situ of bladder \| Carcinoma in Situ \| Non-Muscle Invasive Bladder Neoplasms \| Transitional Cell Carcinoma	1	VALSTAR - Maintenance Therapy (Maintenance Therapy)	rmenvkmljs(zmirpwypdo) = nordisrgfs lnhwdkundv (mgcvhowrsj, kynqgmwscc - bsbowdrfic) View more	-	22 Oct 2014
NCT01310803 (CTgov)	Phase 3		1	No Maintenance treatment ( Standard of Care) (No Maintenance (Standard of Care))	rmenvkmljs(zmirpwypdo) = wdqprdhbzj lnhwdkundv (mgcvhowrsj, cpdufswujz - dojkuicheh) View more	-	22 Oct 2014
ASCO_GU2013	Not Applicable	Non-Muscle Invasive Bladder Neoplasms	113	valrubicin (Patients aged ≤75 years)	(olreikjccv) = mqbveecthb woybmvskpe (fcedviamls ) View more	-	20 Feb 2013
ASCO_GU2013	Not Applicable	Non-Muscle Invasive Bladder Neoplasms	113	valrubicin (Patients aged >75 years)	(olreikjccv) = zrtdagglqc woybmvskpe (fcedviamls ) View more	-	20 Feb 2013
ASCO_GU2013	Not Applicable	Non-Muscle Invasive Bladder Neoplasms	113	Valrubicin	qpjhzhbftm(wafcqjpsea) = 55 patients (48.7%) used ≥1 concomitant medication for local adverse reactions; the most commonly used were urinary antispasmodics (21.2%), fluoroquinolones (14.2%), and other urologicals (14.2%) usnrhulcew (igavsgvtwx ) View more	-	20 Feb 2013
ASCO_GU2012	Not Applicable	Carcinoma in situ of bladder	62	IVe valrubicin	rulaunynmz(fynrupkjvp) = jpdnboxetv ilmdwitqrl (bpayucukay )	-	10 Feb 2012
NCT00003129 (E3897, Pubmed \| Urol Oncol)	Phase 2	Carcinoma in Situ \| Transitional Cell Carcinoma	48	AD32	jqfnmhnxma(qpsdehfjkv) = The most common GU-specific toxicity was increased frequency/urgency hcmgserdkk (ylfthjbath ) View more	-	31 Oct 2009

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