On April 27, 2017 KaloBios Pharmaceuticals, Inc. (OTCQB:KBIO), a biopharmaceutical company focused on advancing medicines for patients with neglected and rare diseases, reported it will change the company’s name to Humanigen, Inc., effective August 7, 2017 (Press release, KaloBios, APR 27, 2017, View Source [SID1234525361]).

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"We have completely transformed into a new company with a focus on neglected and rare disease. Our new identity reflects the company we have re-built with a new team consistently executing our strategy in diseases with high unmet need and leading the way in how we operate," said Cameron Durrant, MD, chairman and CEO. "Moving forward as Humanigen will give us a new platform to continue our significant progress, to focus on the future, and to deliver value for patients, investors and all our other stakeholders."

As Humanigen, the company expects to accelerate this transformation executing on key priorities and anticipated milestones, including:

New Drug Application (NDA) submission for benznidazole in Chagas disease, a neglected tropical disease, to the U.S. Food and Drug Administration (FDA) in first quarter 2018
Submission for both rare pediatric designation and orphan drug designation for lenzilumab in Juvenile Myelomonocytic Leukemia (JMML)
Development of an interim analysis of the lenzilumab Phase 1 trial in Chronic Myelomonocytic Leukemia (CMML)
Up-listing to a national securities exchange and ongoing work to improve the capital structure
In just over a year, the company has transformed how it operates and has rapidly achieved a number of important clinical development milestones, including:

Benznidazole in Chagas disease:

Confirmed that benznidazole is eligible for review via the 505(b)(2) regulatory pathway as a potential treatment for Chagas disease per FDA-issued guidance
Eligible to receive priority review voucher if benznidazole becomes the first FDA-approved treatment for Chagas disease per agency guidance
Opened a benznidazole Investigational New Drug (IND) application with the FDA
Received FDA orphan drug designation for benznidazole
Lenzilumab in CMML:

Initiated a Phase 1 trial of lenzilumab in CMML, a rare disease with unmet need
The company’s stock will also begin trading under the new ticker symbol HGEN on the OTCQB market as of the opening on August 7, 2017 – the effective date. The CUSIP number for Humanigen’s common stock will be 444863104.

The name change does not affect the rights of the company’s stockholders. No action is required by existing stockholders with respect to the name change, and certificates representing outstanding shares of the company’s common stock will not need to be exchanged.

Upon effective date, the company’s website will be www.humanigen.com.

Filed・Approved
As of Mar. 31, 2017
Approved in SG
Filed in HK, MY
◎ARQ 197
Tivantinib
Oral
c-Met Inhibitor
Hepatocellular Cancer
Phase III
in JP
Licensed from
ArQule
Phase Iin JP
Phase IIin US
Phase II in US
Phase II in JP and
KR
Updated since Jan 24th,
2017 （Area, Stage, Filed, Approved, etc.）
◎
R&D Pipeline
Aplastic Anemia
PhaseII/III
in JP and KR
Phase II, Phase III
Central
Nervous
System
KW-6002
Istradefylline
Oral
Adenosine A
2A
Receptor Antagonist
Parkinson’s Disease
Phase III
in US, CA, EU and
others
Phase IIin JP
Phase II
in US, EU and
others
KHK4827
Brodalumab
Injection
Anti-IL-17 Receptor
A Fully Human
Antibody
Psoriasis
Phase III in KR
Nephrology
Area
In-House
Human Antibody-Producing Technology
Jointly Developed with
Ultragenyx in US and EU
X-linked
Hypophosphatemia (XLH)
in pediatric patients
Phase III in US, CA,
EU, AU, JP, KR
Tumor Induced
Osteomalacia(TIO)/Epider
mal Nevus Syndrome
(ENS)
Kirin-Amgen
◎ASKP1240
Bleselumab
Injection
Anti-CD40 Fully
Human Antibody
Organ Transplant
Rejection
In-House
Human Antibody-Producing Technology
Jointly Developed with Astellas
◎KRN23
burosumab
Injection
Anti-FGF23 Fully
Human Antibody
X-linked
Hypophosphatemia(XLH)
in adult patients
Phase III in US, CA,
EU, JP and KR
In-House
◎ＫＷ-6356
Oral
Adenosine A
2A
Receptor Antagonist
Parkinson’s Disease
In-House
Oncology
Jointly Developed with
AstraZeneca/MedImmune
Chronic Obstructive
Pulmonary Disease(COPD)
Phase III in JP
Eosinophilic Chronic
Rhinosinusitis (ECRS)
Phase II in JP
In-House
POTELLIGENT

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Human Antibody-Producing Technology
◎KHK4563
Benralizumab
Injection
Anti-IL-5 Receptor
Humanized Antibody
Asthma
Phase III in JP and
KR
In-House
POTELLIGENT

Immunology
/Allergy
◎KHK4083
Injection
Anti-OX40 Fully
Human Antibody
Ulcerative colitis
KW-0761
Mogamulizumab
Injection
Anti-CCR4
Humanized Antibody
Adult T-cell
Leukemia/Lymphoma
Ph
ase
II
in US, EU and
others
In-House
POTELLIGENT

Cutaneous T-cell
Lymphoma
Phase III
in US, EU, JP and
others
In-House
or
Licensed
Remarks
Licensed from
Reata
◎KHK7580
Evocalcet
Oral
Calcium Receptor
Agonist
Secondary
Hyperparathyroidism
PhaseIII
in JP
Li
cense
d
f
rom
Mitsubishi
Tanabe
Pharma
◎RTA 402
Bardoxolone Methyl
Oral
Antioxidant
Inflammation
Modulator
CKD in Patients with Type
2 Diabetes
PhaseII
in JP
Code Name
Generic Name
Formulation
Mechanism of Action
Indication
Stage
Kirin-Amgen
◎KRN23
burosumab
Injection
Anti-FGF23 Fully
Human Antibody
X-linked
Hypophosphatemia (XLH)
Filed in EU
In-House
Human Antibody-Producing
Technology
Jointly Developed with Ultragenyx
in US and EU
Filed in BN
Licensed from
NPS
Other
AMG531
Romiplostim
Injection
Thrombopoietin
Receptor Agonist
Idiopathic (Immune)
Thrombocytopenic
Purpura
Approved in TH
Licensed from
Solasia Pharma
Z-206
Mesalazine
Oral
pH Dependent
Controlled
Release Tablet
Ulcerative Colitis
(Additional Dosage and
Administration)
Filed in JP
Licensed from
Zeria Pharma
Jointly Developed with Zeria
Pharma
NDA holder is Zeria Pharma
Oncology
Granisetron
Patch
５-HT
3
Serotonin
Receptor Antagonist
Chemotherapy induced
Nausea and Vomiting
Filed in MY
Area
Code Name
Generic Name
Formulation
Mechanism of Action
Indication
Myelodysplastic Syndromes
Kirin-Amgen
KRN321
Darbepoetin Alfa
Injection
Long-Acting
Erythropoiesis
Stimulating Agent
Stage
In-House
or
Licensed
Remarks
Nephrology
Renal Anemia (on Dialysis)
NDA in preparation
in CN
Renal Anemia
Filed in ID
KRN1493
Cinacalcet
Hydrochloride
Oral
Calcium Receptor
Agonist
Secondary
Hyperparathyroidism
Immunology
/Allergy
AMG531
Romiplostim
Injection
Thrombopoietin
Receptor Agonist
Kirin-Amgen
Idiopathic (Immune)
Thrombocytopenic
Purpura
Phase III in CN
Other
New Molecular Entity
Asthma
Filed in JP
In-House
POTELLIGENT

Jointly Developed with
AstraZeneca/MedImmune
NDA holder is AstraZeneca
KHK4827
Brodalumab
Injection
Anti-IL-17 Receptor
A Fully Human
Antibody
Psoriasis
Filed in TW
Kirin-Amgen
◎KHK4563
Benralizumab
Injection
Anti-IL-5 Receptor
Humanized Antibody
antibody
protein
small molecule
Ｐ
h
I
As of Mar.31, 2017
Combination with
Durvalumab/Tremelimumab
(Jointly Developed with AstraZeneca)
Combination with Docetaxel
Combination with
PF-05082566
(Jointly Developed with Pfizer)
Phase I/II
in US
Combination with Nivolumab
(Jointly Developed with Bristol-Myers
Squibb)
PhaseI
in JP
Combination with Nivolumab
(Jointly Developed with
Ono Pharmaceutical)
◎KHK4083
Injection
Anti-OX40 Fully
Human Antibody
Ulcerative colitis
Phase Iin JP
In-House
◎KHK4083
Injection
Anti-OX40 Fully
Human Antibody
Ulcerative colitis
Phase Iin JP
In-House
PhaseIin EU
PhaseIin JP
Updated since Jan 24th,
2017 （Area, Stage, Filed, Approved, etc.）
◎
Updated since Jan 24th,
2017 （Area, Stage, Filed, Approved, etc.）
Filed・Approved
Nephrology
KRN321
Darbepoetin Alfa
Injection
Long-Acting
Erythropoiesis
Stimulating Agent
Myelodysplastic Syndromes Approved in SG Kirin-Amgen
R&D Pipeline
Other
Kirin-Amgen
In-House
or
Licensed
Remarks
Area
Code Name
Generic Name
Formulation
Mechanism of Action
Indication
Stage
KHK4827
Brodalumab
Injection
Anti-IL-17 Receptor
A Fully Human
Antibody
Psoriasis
Filed in TW
AMG531
Romiplostim
Injection
Thrombopoietin
Receptor Agonist
Idiopathic (Immune)
Thrombocytopenic
Purpura
Approved in TH
Immunology
/Allergy
In-House
POTELLIGENT

Jointly Developed with
AstraZeneca/MedImmune
NDA holder is AstraZeneca
◎KHK4563
Benralizumab
Injection
Anti-IL-5 Receptor
Humanized Antibody
Asthma
Filed in JP
Kirin-Amgen
In-House
Others
KW-3357
Antithrombin
Gamma
Injection
Recombinant Human
Antithrombin
Disseminated Intravascular
Coagulation, Congenital
Antithrombin Deficiency
Phase Iin EU
Licensed from
Immunas
Pharma
Immunology/
Allergy
POTELLIGENT

Human Antibody-Producing Technology
POTELLIGENT

Human Antibody-Producing Technology
PhaseI
in US
Remarks
POTELLIGENT

Human Antibody-Producing Technology
KW-0761
Mogamulizumab
Injection
Anti-CCR4
Humanized Antibody
Solid Tumor
Phase I
in US
In-House
POTELLIGENT

◎KHK2823
Injection
Anti-CD123 Fully
Human Antibody
Cancer
Phase I
in UK
In-House
In-House
Combination with KW-0761
PhaseI
in JP
Syndax
領域
Code Name
Generic Name
Formulation
Mechanism of Action
Indication
Stage
In-House
or
Licensed
◎KHK2455
Oral
IDO 1 Inhibitor
Solid Tumor
New Molecular Entity
Oncology
◎KHK2375
Entinostat
Oral
HDAC Inhibitor
Breast Cancer
Central
Nervous
System
◎KHK6640
Injection
Anti–Amyloid Beta
Peptide Antibody
Alzheimer’s Disease
antibody
protein
small molecule

On April 17, 2017 PIQUR Therapeutics AG, a Swiss clinical-stage pharmaceutical company, reported that
the European Medicines Agency (EMA) has granted orphan drug designation to PIQUR’s lead compound PQR309 for the treatment of patients with diffuse large B-cell lymphoma (DLBCL) (Press release, PIQUR Therapeutics, APR 27, 2017, View Source content/uploads/2017/04/PIQUR_MediaRelease_EMA_OrphanDrug_EN_20170427.pdf [SID1234527271]).

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"The EMA orphan drug designation for PQR309 in DLBCL is another important regulatory milestone, validating the potential therapeutic use of PQR309 in DLBCL," said Claudia Pluess, Senior Regulatory Affairs Manager at PIQUR. Dr. Vladimir Cmiljanovic, CEO of PIQUR, added, "PIQUR will continue to work with physicians and regulatory agencies to further define the clinical development strategy to bring a potential new treatment option to patients suffering
from this disease."

DLBCL is an aggressive form of lymphoma, and the most common type of non-Hodgkin lymphoma (NHL), accounting for about 30 percent of all NHL cases [1]. The disease occurs primarily in older individuals, though it can also occur in children and young adults in rare cases. 10 to 15 percent of DLBCL patients exhibit refractory disease and an additional 20 to 25 percent relapse after initial response to therapy [2].

In addition to this orphan drug designation by the EMA in DLBCL, PIQUR has also recently received orphan drug designation from the FDA for PQR309 for the treatment of primary CNS lymphoma (PCNSL).

The EMA orphan drug designation is a status assigned to a medicine intended for use against a rare condition (prevalence of the condition in the European Union must not be more than 5 in 10,000) and allows a pharmaceutical company to benefit from incentives offered by the EU to develop a medicine for the treatment, prevention or diagnosis of a disease that is life threatening or a chronically debilitating rare disease.

About PQR309
PIQUR’s lead compound, PQR309, is an oral, brain-penetrant, dual inhibitor of the PI3K/mTOR pathway, which is activated in 60 – 80% of human cancers. Unlike most of its competitors, PQR309 crosses the blood-brain barrier, expanding its use to malignant diseases involving the brain. PQR309 has shown both preclinical activity in various tumor models and clinical activity in Phase 1 and 2 studies.

PQR309 is currently being investigated in several Phase 1 and 2 clinical studies in advanced solid tumors (NCT02483858), relapsed or refractory lymphoma (NCT02249429), relapsed or refractory PCNSL (NCT02669511) and progressive glioblastoma multiforme (NCT02850744). In addition, the PIQHASSO Phase 1/2b study investigates PQR309 in combination with Eisai’s Eribulin in metastatic HER2-negative and triple-negative breast cancer (NCT02723877). Additional information regarding the PQR309 clinical trials is available on
www.clinicaltrials.gov.

Alder Biopharmaceuticals has filed a 10-Q – Quarterly report [Sections 13 or 15(d)] with the U.S. Securities and Exchange Commission (Filing, 10-Q, Alder Biopharmaceuticals, 2017, APR 27, 2017, View Source [SID1234521703]).

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On April 26, 2017 Silvergate Pharmaceuticals, Inc. (www.silvergatepharma.com), leaders in the development and commercialization of innovative and safe medicines for children, reported that the United States Food and Drug Administration (FDA) approved XATMEP (methotrexate) Oral Solution, the first and only FDA-approved methotrexate oral solution (Press release, Silvergate Pharmaceuticals, APR 26, 2017, View Source [SID1234625387]). XATMEP is indicated for the treatment of acute lymphoblastic leukemia (ALL) and polyarticular juvenile idiopathic arthritis (pJIA) in pediatric patients.

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"XATMEP is an exciting product in that it provides an FDA-approved, ready-to-use oral solution of methotrexate for children without the need for needles, crushing of tablets or compounding into a liquid formulation," said Frank Segrave, President & CEO, Silvergate Pharmaceuticals, Inc. "As a company, we continue to focus on pediatric medications that are safe, effective, and readily available."

XATMEP (methotrexate) Oral Solution, 2.5 mg/mL, is a ready-to-use product that requires no preparation, facilitating accuracy and ease of dispensing at the pharmacy. XATMEP is manufactured under CGMPs in accordance with FDA regulations. It eliminates the need for needles, crushing or splitting tablets or for compounding tablets into a liquid formulation. It requires refrigeration but may be stored at room temperature for 60 days after dispensing. XATMEP is available through an extensive network of pharmacies and a qualified mail-order service. For additional information on how to obtain XATMEP, please call 1-855-379-0382.

INDICATIONS

XATMEP is a folate analog metabolic inhibitor indicated for the:

management of pediatric patients with active polyarticular juvenile idiopathic arthritis (pJIA) who have had an insufficient therapeutic response to, or are intolerant of, an adequate trial of first-line therapy including full dose non-steroidal anti-inflammatory agents (NSAIDs).
treatment of pediatric patients with acute lymphoblastic leukemia (ALL) as part of a multi-phase, combination chemotherapy maintenance regimen.
About XATMEP

XATMEP (methotrexate) Oral Solution was developed, primarily, to meet the need for a ready-to-use, 2.5 mg/mL, methotrexate oral solution for the treatment of pediatric patients for the indications stated above. Currently, there is no FDA-approved, ready-to-use oral liquid formulation of methotrexate for use by pediatric patients requiring body surface area (BSA) dosing (mg/m2) or who have difficulty swallowing or cannot consume tablets, or those with needle-phobia. Silvergate Pharmaceuticals, Inc.’s XATMEP (methotrexate) Oral Solution resolves these unmet medical needs in pediatric patients.

IMPORTANT SAFETY INFORMATION

XATMEP includes a BOXED WARNING: SEVERE TOXIC REACTIONS, INCLUDING EMBRYO-FETAL TOXICITY

See full prescribing information for complete boxed warning.

Methotrexate can cause severe or fatal toxicities. Monitor closely and modify dose or discontinue for the following toxicities: bone marrow suppression (5.1), infection (5.2), renal (5.3), gastrointestinal (5.4), hepatic (5.5), pulmonary (5.6), hypersensitivity and dermatologic (5.7).
Methotrexate can cause embryo-fetal toxicity and fetal death. Use in polyarticular juvenile idiopathic arthritis is contraindicated in pregnancy (4). Consider the benefits and risks of XATMEP and risks to the fetus when prescribing XATMEP to a pregnant patient with a neoplastic disease. Advise patients to use effective contraception during and after treatment with XATMEP (5.9, 8.1, 8.3).
ADDITIONAL IMPORTANT SAFETY INFORMATION

XATMEP is contraindicated in patients who are hypersensitive to methotrexate.
XATMEP is contraindicated in patients who are pregnant or nursing.
Warnings and Precautions:

Monitor closely and modify dose or discontinue XATMEP as appropriate.

Methotrexate can cause the following severe, life-threatening or fatal adverse reactions:

Bone marrow suppression: pancytopenia, anemia, leukopenia, neutropenia, and thrombocytopenia.
Serious infections: bacterial, fungal, or viral infections, including Pneumocystis jiroveci pneumonia, invasive fungal, hepatitis B reactivation, tuberculosis, Herpes zoster and cytomegalovirus infections.
Renal toxicity and renal impairment, including acute renal failure.
Gastrointestinal toxicity: diarrhea, stomatitis, vomiting, hemorrhagic enteritis, fatal intestinal perforation. Unexpected severe and fatal gastrointestinal toxicity can occur with concomitant us of NSAIDs.
Hepatic toxicity: severe and potentially irreversible hepatotoxicity, including fibrosis, cirrhosis, and fatal liver failure.
Pulmonary toxicity: acute or chronic interstitial pneumonitis and irreversible or fatal cases at all dose levels.
Hypersensitivity: anaphylaxis.
Dermatologic reactions: toxic epidermal necrolysis, Stevens-Johnson syndrome, exfoliative dermatitis, skin necrosis, erythema multiforme. Radiation dermatitis and "sunburn" may be recalled.
Secondary malignancies: lymphoproliferative disease has been reported with low-dose oral methotrexate which regressed when methotrexate is withdrawn.
Embryo-fetal toxicity and fetal death: Consider the risks and benefits of XATMEP and risks to the fetus when prescribing to a pregnant patient with a neoplastic disease. XATMEP is contraindicated in non-neoplastic disease.
Immunizations may be ineffective when given during XATMEP therapy.
Immunization with live virus vaccines is not recommended during XATMEP therapy.
Effects on reproduction: Methotrexate can cause impairment of fertility, oligospermia, and menstrual dysfunction. Effective contraception should be practiced by patients of reproductive potential while receiving XATMEP therapy, and for 3 and 6 months afterwards for males and females, respectively.
Third-space accumulation: Evacuate significant third-space accumulation prior to methotrexate administrations.
Concomitant radiation therapy increases the risk of soft tissue necrosis and osteonecrosis associated with methotrexate.
Closely monitor laboratory parameters for hematology, renal function and liver function. Increase monitoring during initial dosing, dose changes and during periods of increased risk of elevated methotrexate blood levels (e.g., dehydration).
Improper dosing: Once weekly dosing is appropriate. Fatal toxicity has been reported with daily dosing. An accurate millimeter measuring device should be used.
Advise women not to breastfeed.
Adverse Reactions: See full prescribing information for additional adverse reactions.

Most common adverse reactions are ulcerative stomatitis, leukopenia, nausea, abdominal distress, and elevated liver function tests.

Other frequently reported reactions are malaise, fatigue, chills and fever, dizziness, and decreased risk to infection.

Drug Interactions:

Oral antibiotics: Hematologic and gastrointestinal toxicity may increase.
Hepatotoxins: May increase hepatoxicity.
Probenecid: Consider alternative drugs as may increase methotrexate exposure.
Theophylline: May reduce theophylline clearance.
To report SUSPECTED ADVERSE REACTIONS, contact Silvergate Pharmaceuticals at 1-855-379-0383, or FDA at 1-800-FDA-1088 or www.fda.gov/MedWatch.

Please see accompanying full Prescribing Information, including the complete BOXED WARNING.

About Silvergate Pharmaceuticals, Inc.
Headquartered near Denver, Colorado, Silvergate Pharmaceuticals, Inc., is a privately held pharmaceutical company dedicated to leading the way in the development and commercialization of innovative pediatric medications that are safe, effective, and readily available.

Silvergate Pharmaceuticals is committed to filling the unmet needs of children, developing innovative medications that will help improve the quality of care and outcomes for pediatric patients. For more information, please visit View Source

Reference: XATMEP [prescribing information]. Greenwood Village, CO: Silvergate Pharmaceuticals, Inc.; 2017.