On December 7, 2018 Sophiris Bio Inc. (the "Company") reported that entered into an Controlled Equity OfferingSM Sales Agreement (the "Sales Agreement") with Cantor Fitzgerald & Co., as sales agent ("Cantor Fitzgerald"), pursuant to which the Company may offer and sell, from time to time, through Cantor Fitzgerald, common shares of the Company having an aggregate offering price of up to $20.0 million (Press release, Sophiris Bio, DEC 7, 2018, View Source [SID1234531962]). The shares will be offered and sold pursuant to the Company’s shelf registration statement on Form S-3 (File No. 333-219887).

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The Company is not obligated to sell any shares under the Sales Agreement. Subject to the terms and conditions of the Sales Agreement, Cantor Fitzgerald will use commercially reasonable efforts, consistent with its normal sales and trading practices, applicable state and federal law, rules and regulations and the rules of the Nasdaq Capital Market, to sell shares from time to time based upon the Company’s instructions, including any price, time or size limits specified by the Company. Under the Sales Agreement, Cantor Fitzgerald may sell shares in privately negotiated transactions or by any other method or payment permitted by law deemed to be an "at-the-market" offering as defined in Rule 415 under the Securities Act of 1933, as amended. The Company will pay Cantor Fitzgerald a commission of 3.0% of the aggregate gross proceeds from each sale of shares, reimburse certain legal fees and disbursements and provide Cantor Fitzgerald with customary indemnification and contribution rights. The Sales Agreement may be terminated by Cantor Fitzgerald or the Company at any time upon notice to the other party, or by Cantor Fitzgerald at any time in certain circumstances, including the occurrence of a material and adverse change in the Company’s business or financial condition that makes it impractical or inadvisable to market the shares or to enforce contracts for the sale of the shares.

The foregoing description of the Sales Agreement does not purport to be complete and is qualified in its entirety by reference to the full text of the Sales Agreement, a copy of which is filed as Exhibit 10.1 to this Current Report on Form 8-K. The legal opinion of Fasken Martineau DuMoulin LLP relating to the common shares being offered pursuant to the Sales Agreement is filed as Exhibit 5.1 to this Current Report on Form 8-K.

This Current Report on Form 8-K shall not constitute an offer to sell or the solicitation of an offer to buy any shares under the Sales Agreement, nor shall there be any sale of such shares in any state in which such offer, solicitation or sale would be unlawful prior to registration or qualification under the securities laws of any such state.

On December 7, 2018 Agendia, Inc., a world leader in precision oncology, reported findings from two key studies presented at the 2018 San Antonio Breast Cancer Symposium (SABCS) this week, reinforcing the utility and benefits of its MammaPrint 70-Gene Breast Cancer Risk-of-Recurrence and BluePrint Breast Cancer Molecular Subtyping tests (Press release, Agendia, DEC 7, 2018, View Source [SID1234531959]). Both studies underscore the growing importance of genomic testing in helping physicians to personalize breast cancer treatment management.

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BluePrint reclassifies 85 percent of HER2-positive, and clarifies HER2-equivocal breast cancers in a real-world diagnostic setting1

The first study addressed challenges acknowledged within the Aphinity and ExteNET trials regarding the potential benefits of added HER2-targeted treatment in breast cancer as well as the uncertainty regarding the nature of tumors classified as HER2 "equivocal" by traditional immunohistochemistry (IHC) and fluorescence in situ hybridization (FISH). A previous trial showed that BluePrint reclassified almost half of HER2-postive/ER-positive patients identified as HER2-positive using IHC/FISH to the Luminal subtype with differential neoadjuvant treatment response.2,3

In this study, Agendia scientists analyzed HER2-positive and HER2-equivocal cancers (as defined by the 2013 CAP Guidelines), comparing IHC/FISH status from pathology results to BluePrint molecular subtype in a real-world diagnostic setting. In IHC/FISH HER2-amplified tumors, BluePrint reclassified 85 percent to non-HER2 molecular subtypes, mostly Luminal-type for ER-positive tumors and Basal-type for ER-negative tumors. BluePrint also classified all HER2-equivocal tumors to non-HER2 subtypes, Luminal and Basal, which could not be derived from IHC/FISH. No HER2 "equivocal" cancers by IHC/FISH displayed a HER2-driven genotype.

Dr. William Audeh, chief medical officer at Agendia, said: "The findings from this real-world study indicate that additional therapeutic options should be considered for some women with clinically HER2-positive cancers with genomic profiles of Luminal or Basal subtypes. These data also provide further precision to clarify the clinical uncertainty regarding the HER2 "equivocal" subtype. This study further reinforces the critical role BluePrint plays in helping to inform more personalized treatment decisions by adding to a growing body of evidence demonstrating the importance of tumor molecular subtyping in breast cancer."

MammaPrint identifies 46 percent of patients under 50 years of age with an intermediate recurrence score as Low Risk4

The second study reevaluated data from the PROMIS (PRospective Study Of MammaPrint in Patients With an Intermediate Recurrence Score) trial using the same subgroup analyses that was used in the TAILORx trial. It aimed to establish greater certainty regarding the benefits of chemotherapy among female breast cancer patients under 50 with an intermediate recurrence score from the 21-gene assay (RS 18-30). The new analyses found 46 percent of these women had a low genomic risk of recurrence as assessed by MammaPrint and were unlikely to benefit from chemotherapy. Researchers also found that in the MINDACT trial, MammaPrint patients younger than age 45 and between the ages of 45-55 who also have a Low Risk result had a favorable 5-year distant metastasis-free survival of 95-98 percent in both clinically low and high risk groups.

Dr. Hatem Soliman, medical director of clinical trials at the Moffitt Cancer Center and lead study author, said: "The TAILORx trial raised important questions about the benefits of chemotherapy in women under 50, so we were pleased to see that our new subgroup analysis of the PROMIS data, using the same approach as seen in TAILORx, showed that MammaPrint provides greater certainty regarding which women are unlikely to benefit from chemotherapy. Patient quality of life, in the short-term and longer-term, is paramount, so the role of MammaPrint in signaling where physicians can safely de-escalate their patients’ treatments, and thus side effects, is important."

A full list of abstracts featuring MammaPrint and BluePrint presented during SABCS can be viewed here: View Source(2018NOV)%20-%20SABCS%202018%20Abstract%20Summary%20interactive.pdf

1. BluePrint molecular subtyping versus HER2 assessment by immunohistochemistry and FISH in the real-world diagnostic setting. Poster presented at SABCS. December 2018; San Antonio, Texas.

2. Whitworth P, et al., Chemosensitivity Predicted by BluePrint 80-Gene Functional Subtype and MammaPrint in the Prospective Neoadjuvant Breast Registry Symphony Trial (NBRST). Ann Surg Oncol. 2014; 21(10): 3261–3267.

3. Pathological complete response in basal subtype tumors predicts improved distant metastasis free survival in the NBRST trial. Poster presented at ASCO (Free ASCO Whitepaper) 2018; Chicago, Illinois.

4. MammaPrint identifies 46% of patients, age ≤50 years with oncotype RS 18-30, as low risk and safe to forgo chemotherapy. Poster presented at SABCS. December 2018; San Antonio, Texas.

About MammaPrint

MammaPrint is an in vitro diagnostic medical device, performed as a testing service in a central laboratory, using the 70-gene expression profile of breast cancer tissue samples to assess a patient’s risk for distant metastasis. The device is FDA-cleared and CE-marked, enabling use in the European Union. MammaPrint is indicated for use by physicians as a prognostic marker only, along with other clinical-pathological factors. It is not intended to determine the outcome of disease, nor to suggest or infer an individual patient’s response to therapy. MammaPrint is the only test of its kind recommended for lymph node-negative and lymph node-positive patients by both the American Society of Clinical Oncology (ASCO) (Free ASCO Whitepaper) and National Comprehensive Cancer Network (NCCN). The test is also recommended by many other national and international clinical practice guidelines.

On December 7, 2018 Biologics by McKesson, an independent specialty pharmacy for oncology and other complex therapeutic areas, reported that it has been selected by Astellas Pharma US, Inc. to be in the limited distribution network for XOSPATA (gilteritinib) (Press release, McKesson, DEC 7, 2018, View Source [SID1234531958]).

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XOSPATA is indicated for the treatment of adult patients who have relapsed or refractory Acute Myeloid Leukemia (AML) with a FMS-like tyrosine kinase 3 (FLT3) mutation as detected by an FDA-approved test. XOSPATA was approved by the U.S. Food and Drug Administration (FDA) on November 28, 2018, based on an interim analysis of data from the ongoing phase III ADMIRAL trial. In May 2018, the FDA accepted, with Priority Review, the company’s New Drug Application (NDA) for gilteritinib. Previously, gilteritinib was granted both Orphan Drug designation and Fast Track designation by the FDA.

Acute Myeloid Leukemia (AML) is a cancer that impacts the blood and bone marrow, and its incidence increases with age. The American Cancer Society estimates that in 2018, approximately 19,000 new patients will be diagnosed with AML in the U.S. XOSPATA is the first and only FLT3-targeting agent approved by the FDA for the treatment of adult patients with relapsed or refractory FLT3 mutation-positive (FLT3mut+) AML.

"Patients with FLT3 mutation–positive relapsed or refractory acute myeloid leukemia have had limited treatment options," said Brandon Tom, PharmD, vice president, Commercial Services, Biologics by McKesson. "We are pleased to be able to offer this much needed new drug to this patient population, who accounts for approximately 30 percent of all AML patients."

Biologics by McKesson is committed to and recognized for its high level of customer service as well as its innovative, high-touch and multidisciplinary patient-centric approach. Each team includes a pharmacist with in-depth knowledge of oncology therapies, an experienced oncology nurse and a financial counselor who is familiar with various financial assistance programs and organizations that help cancer patients. This highly-skilled care team works together to develop individualized care plans that address each patient’s unique clinical, financial and emotional needs and streamlines communication back to the treating provider, enabling high-quality care and differentiated outcomes. In addition, the Biologics by McKesson team works closely with payers to ensure patients can access the specialty medications they need.

Physicians may submit prescriptions to Biologics by McKesson via phone (800.850.4306), fax (800.823.4506) or eScribe. For electronic prescribing systems, physicians may search for Biologics within their EMR system.

On December 7, 2018 Bio-Thera Solutions, a clinical-stage pharmaceutical company, reported that patient dosing has begun in a Phase I clinical study of BAT4306F in relapsed/refractory CD20-positive B-cell non-Hodgkin’s lymphoma patients. BAT4306F is an ADCC-enhanced CD20 monoclonal antibody that has demonstrated enhanced potency in preclinical studies with potential to be a "best-in-class" therapeutic (Press release, BioThera Solutions, DEC 7, 2018, View Source [SID1234531957]).

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"Initiating our Phase I clinical trial for BAT4306F represents a major milestone for Bio-Thera Solutions as BAT4306F is our first clinical candidate developed for the treatment of hematologic malignancies," said Shengfeng Li, CEO, Bio-Thera Solutions. "While the BAT4306F development plan will be initially focused on CD20-positive B-cell non-Hodgkin’s lymphoma we believe BAT4306F also has great potential as a treatment for other hematologic malignancies."

The Phase 1, multicenter, open-label, dose-escalation clinical trial of BAT4306F is designed to assess the safety and tolerability of BAT4306F as a single agent. The study will enroll subjects with relapsed/refractory CD20-positive B-cell non-Hodgkin’s lymphoma. Key objectives in the study include determining maximum tolerated dose, dose-limiting toxicity, pharmacokinetics and recommended doses for phase II clinical studies.

More information on the trial is available at View Source (CTR20181568).

About BAT4306F

BAT4306F is an investigational ADCC-enhanced CD20 monoclonal antibody that has the potential to be a "best-in-class" therapeutic. BAT4306F is currently being evaluated in relapsed/refractory CD20-positive B-cell non-Hodgkin’s lymphoma. CD20 is a naturally occurring receptor that is overexpressed in many types of hematologic malignancies. BAT4306F is being developed for use as a single agent and in combination with other agents for a variety of hematologic malignancies.

on December 7, 2018 Janssen Pharmaceutical Companies of Johnson & Johnson reported new results from three key studies on IMBRUVICA (ibrutinib) for Chronic Lymphocytic Leukemia (CLL), a form complex to treat blood cancer and the most common form of leukemia in adults (Press release, Johnson & Johnson, DEC 7, 2018, View Source [SID1234531955]). 1 The findings were presented at the 60 th Annual Meeting of the American Society of Hematology (ASH) (Free ASH Whitepaper) in San Diego, California.

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The results of the National Cancer Institute (NCI) Phase 3 study (E1912), led by the ECOG-ACRIN Cancer Research Group (ECOG-ACRIN), were presented during the oral session on last-minute abstracts . The study evaluated ibrutinib plus rituximab compared to a chemotherapy regimen with fludarabine, cyclophosphamide and rituximab (FCR) in previously untreated patients aged 70 years or less with CLL. With nearly three years of follow-up, data showed that ibrutinib plus rituximab significantly prolonged progression-free survival (PFS) and overall survival (OS) compared with CRF. 2

Phase III data from the iLLUMINATE (PCYC-1130) study were also presented at an oral session and published simultaneously in The Lancet Oncology . The findings showed that the combination of ibrutinib plus obinutuzumab significantly improved PFS compared with chlorambucil plus obinutuzumab in patients with newly diagnosed CLL. 3 These data have recently supported a request for Type II variation filed with the European Medicines Agency (EMA) and aimed at approval for the expanded use of ibrutinib in combination with obinutuzumab in adults not previously treated with

In addition, data on ibrutinib in the Phase 1b / 2 study and its extension study (PCYC-1102, PCYC-1103) with follow-up of up to 7 years in patients with CLL recently diagnosed recurrent / refractory (R / R) have demonstrated long-term, sustainable survival benefits in monotherapy, the longest follow-up for a Bruton tyrosine kinase (BTK) inhibitor in the treatment of an LLC. 4

"The results of the iLLUMINATE and ECOG-ACRIN studies demonstrate an impressive increase in progression-free survival for relevant ibrutinib-based combinations, compared to the commonly used chemo-immunotherapy protocols," says hematologist consultant Dr. Carol Moreno. at the Santa Creu Sant Pau Hospital, Autonomous University of Barcelona, ​​Barcelona, ​​Spain. "These chemotherapy-free protocols represent a breakthrough in our approach to treating patients, including young patients and those with high-risk CLL, with the potential to reach a compromise between efficacy and patient toxicity. . "

"The data presented at the ASH (Free ASH Whitepaper) provide convincing additional evidence of the clinical benefit that ibrutinib can provide to patients across all CLL therapies." Long-term data provide confidence for its prolonged activity for patients, "says Dr. Catherine Taylor, Head of Hematology Therapies for Europe, Middle East and Africa (EMEA) at Janssen-Cilag Limited. "We continue to explore the full potential of ibrutinib through a comprehensive clinical development program, to improve outcomes and change what a diagnosis of blood cancer can mean for patients."

Ibrutinib, a leading BTK inhibitor, is jointly developed and marketed by Janssen Biotech, Inc., and Pharmacyclics LLC, an AbbVie company.

Results of the Randomized Phase 3 Study of Ibrutinib-Based Therapy (PCI-32765) vs FCR Chemo-Immunotherapy in Young Untreated CLL Patients: An ECOG-ACRIN Cancer Study Research Group (E1912) ( Abstract No. LBA-4 )

With a median follow-up of 33.4 months, the interim analysis observed 77 PHC events and 14 deaths. Ibrutinib plus rituximab significantly improved PFS compared with RCF (RR 0.352, 95 percent confidence interval [CI] 0.223-0.558, p <0.0001); the pre-specified threshold for the SSP has been crossed. The ibrutinib plus rituximab group also showed an improvement in SG (RR: 0.168, 95 percent CI: 0.053-0.538, p = 0.0003, pre-specified threshold for superiority p = 0.0005). 2

In a subgroup analysis for PFS, ibrutinib plus rituximab showed lengthening of PFS regardless of age, gender, performance status, stage of illness, or presence / absence of the cytogenetic abnormality, deletion 11q23. According to current monitoring, ibrutinib plus rituximab was also superior to CRF for non-mutated IGHV patients (RR: 0.262, 95 percent CI 0.137-0.498, p <0.0001), but not IGHV patients mutated (RR 0.435, 95 percent CI 0.140-0.11350, p = 0.07). 2

Grade 3/4 treatment-related adverse events were observed in 58 percent of patients treated with ibrutinib plus rituximab, and 72 percent of patients treated with CRF (p = 0.0042). The RCF was more frequently associated with grade 3 and 4 neutropenia (RCF: 44 percent vs ibrutinib plus rituximab: 23 percent, p <0.0001) and infectious complications (RCF: 17.7 percent vs ibrutinib plus rituximab: 7.1 percent, p <0.0001). 2

Results of the iLLUMINATE Phase 3 study ( abstract n ° 691 )

At a median follow-up of 31.3 months, ibrutinib plus obinutuzumab had significantly lengthened the PFS assessed by an independent review committee (IRC), compared with chlorambucil plus obinutuzumab (mean unmet vs. 19.0 months; 0.231, 95 percent CI 0.145-0.367, p <0.0001), with a 77 percent reduction in the risk of progression or death. 3

A higher SSP in the ibrutinib plus obinutuzumab group, compared to the chlorambucil plus obinutuzumab group, was also observed in the high risk group, including in patients with IGHV, del11q, del17p non-mutated and / or TP53 mutation, with 85 percent reduction in risk of progression or death (mean not achieved vs. 14.7 months, RR 0.154, 95 percent CI: 0.087-0.270, p <0.0001). 5 In addition, the overall response rate (TRG) assessed by CEI was higher in the ibrutinib plus obinutuzumab group compared to the chlorambucil plus obinutuzumab group (88 percent vs. 73 percent); Complete response rates (CR) / complete response with incomplete blood recovery were also higher (19 percent vs. 8 percent, respectively). Minimal residual disease (MRM) was not detectable in the blood and / or bone marrow (<10 -4 by flow cytometry) for 35 percent of patients treated with ibrutinib plus obinutuzumab, compared to 25 percent of patients treated with chlorambucil plus obinutuzumab. The 30-month SG rates were 86 percent for the ibrutinib plus obinutuzumab group compared to 85 percent for the chlorambucil plus obinutuzumab group. 3

The most common grade 3 or higher adverse events in the ibrutinib plus obinutuzumab group, compared to the chlorambucil plusobinutuzumab group, were neutropenia (36 percent vs 46 percent), thrombocytopenia (19 percent vs. 10 percent) pneumonia (7 percent vs. 4 percent), atrial fibrillation (5 percent vs. 0 percent), febrile neutropenia (4 percent vs. 6 percent), anemia (4 percent vs. 8 percent), and perfusion (PRP, 2 percent vs 8 percent). 5No patients stopped taking obinutuzumab because of RLP in the ibrutinib plus obinutuzumab group, compared to the chlorambucil plus obinutuzumab group (6 percent). Adverse events led to discontinuation of ibrutinib in 16 percent of patients, and discontinuation of chlorambucil in nine percent of patients. Adverse events led to discontinuation of obinutuzumab in the ibrutinib plus obinutuzumab group (9 percent) and in the chlorambucil plus obinutuzumab group (13 percent). With approximately three years of follow-up, 70 percent of patients in the ibrutinib plus obinutuzumab group continue ibrutinib monotherapy. 3

Follow-up Results to Seven Years in PCYC-1102 Phase 1b / 2 and its Extension Study, PCYC-1103 ( Abstract # 3133 )

The results of these studies demonstrated the sustained efficacy of ibrutinib in patients with newly diagnosed R / R LLC. These long-term data showed prolonged PHC and OS. The estimated seven-year PHC rates were 80 percent for patients with newly diagnosed disease and 32 percent for patients with R / R disease. It should be noted that earlier administration of ibrutinib in the therapeutic lines resulted in an improvement in SSP for R / R patients. 4

The TRG was 89 percent for all patients (RC, 15 percent), with similar rates in newly diagnosed patients (87 percent [RC, 32 percent]) and R / R LLC patients (89 percent). cent [RC, 10 percent]). The median response time (DR) was not reached (95 percent CI: 0 + -85 +) for newly diagnosed CLL patients and was 57 months (95 percent CI: 0 + – 85+) for R / R LLC patients. 6 Median PFS was not achieved (95 percent CI: not estimable [NE], NE) for newly diagnosed CLL patients, and 51 months (95 percent CI 37-70) for R / R LLC patients. 4.6Median OS was not affected in newly diagnosed patients (95 percent of IC: 80-NE) or in R / R LLC patients (95 percent of IC: 63-NE), with seven-year GS estimates of 75 percent and 52 percent, respectively. 4

Grade 3 or higher adverse events were reported in 74 percent of newly diagnosed patients and 89 percent of R / R LLC patients. Of the Grade 3 or higher adverse events that occurred during treatment, the most common were: hypertension (newly diagnosed, 32 percent, R / R, 26 percent), diarrhea (newly diagnosed, 16 percent, R / R , 4 percent), and hyponatraemia (newly diagnosed, 10 percent, R / R, 0 percent). Cases of major bleeding and atrial fibrillation, thrombocytopenia, anemia, and grade 3 or greater arthralgia have been observed in 11 percent or less of newly diagnosed patients and R / R patients. In addition, the cases of6 No new or unexpected adverse events were observed, and the occurrence of most grade 3 or higher adverse events and serious adverse events decreased over time, with the exception of hypertension. 6

#END#

About the ECOG-ACRIN E1912 study

The Phase 3 study (E1912) evaluated previously untreated CLL patients aged 70 years or less who were randomized to receive ibrutinib (420 mg / day until disease progression) and rituximab (50 mg / m 2 at day 1 of cycle 2, 325 mg / m 2 at day 2 of cycle 2, 500 mg / m 2 at day 1 of cycles 3-7) (n = 354) or six series intravenous fludarabine (25 mg / m 2 ) and cyclophosphamide (250 mg / m 2 ) on days 1-3 with rituximab (50 mg / m 2 on day 1 of cycle 1, 325 mg / m 2 on day 2 Cycle 1, 500 mg / m 2at day 1 of cycles 2-6) every 28 days (n = 175). The main criterion was SSP, with the SG as a secondary criterion. 2

From federal funding, the study was designed by ECOG-ACRIN researchers. It was conducted via NCI’s national clinical trial network. Pharmacyclics LLC provided ibrutinib as part of a cooperative research and development agreement with the NCI and a separate agreement with ECOG-ACRIN.

About the iLLUMINATE study

The iLLUMINATE study ( PCYC-1130 ) evaluated patients with newly diagnosed CLL who were randomized to receive ibrutinib 420 mg once daily continuously until disease progression or unacceptable toxicity in combination with obinutuzumab 1000 mg intravenous for six cycles (n = 113); or chlorambucil on days 1 and 15 of each cycle plus obinutuzumab 1000 mg intravenously for 6 cycles (n = 116). The median age of the patients was 71 years and 65 percent of the patients had high risk genomic characteristics. The primary criterion was SSP, as assessed by an independent review committee. Secondary endpoints included PHC in a high-risk population,3

About PCYC-1102 and PCYC-1103 studies

With follow-up up to seven years, studies (Phase 1b / 2, PCYC-1102 and its extension study, PCYC-1103 ) evaluated patients with newly diagnosed R / R CLL (n = 132; diagnosed = 31, R / R = 101), including patients with high-risk characteristics, who received 420 mg or 840 mg ibrutinib once daily until disease progression or unacceptable toxicity. At the cutoff date, 55 percent of newly diagnosed patients and 21 percent of R / R patients had continued ibrutinib, with a median follow-up of 67 months. 4

About ibrutinib

Ibrutinib is a first-of-its-kind Bruton tyrosine kinase inhibitor (BTK), which acts as a strong covalent bond to BTK to block the transmission of cell survival signals into malignant B-cells. 7 By blocking this BTK protein, ibrutinib helps kill and reduce the number of cancer cells, thus delaying cancer progression. 8

The Ibrutinib is currently approved in Europe for the following uses: 9

Chronic Lymphocytic Leukemia (CLL): as a single agent in the treatment of adult patients with previously untreated CLL, and as a single agent or in combination with bendamustine plus rituximab (BR) for treatment adult patients with CLL who have received at least one therapy.
Mantle lymphoma: adult patients with recurrent or refractory mantle cell lymphoma.
Waldenström Macroglobulinemia (WM): Adult patients who have received at least one therapy or first-line treatment for patients not eligible for chemo-immunotherapy.
Ibrutinib is approved in more than 90 countries and has been used to date to treat more than 135,000 patients worldwide on all of its approved indications. 10

The most common adverse reactions observed with ibrutinib were: diarrhea, neutropenia, hemorrhage (eg bruising), musculoskeletal pain, nausea, rash, and pyrexia. 9

For a complete list of side effects and for information on dosage and administration, contraindications and other precautions on the use of ibrutinib, please refer to the summary of product characteristics .