On October 12, 2021 NanoString Technologies, Inc. (NASDAQ: NSTG), a leading provider of life science tools for discovery and translational research, reported the launch of the nCounter ADC Development Panel, a specialized gene expression tool for use in the rapidly expanding field of Antibody Drug Conjugates (ADCs) (Press release, NanoString Technologies, OCT 12, 2021, View Source [SID1234591154]). Created in collaboration with leading pharmaceutical and clinical scientists, this novel panel is designed to provide molecular insights into important biological questions and challenges of oncology therapies.

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ADCs are defined as a new class of highly potent therapeutics composed of an antibody attached via a chemical linker to a biologically active drug or cytotoxic compound. These targeted agents allow for sensitive discrimination between healthy and cancer tissues with the cell-killing ability of cytotoxic drugs. The field now has 10 approved drugs, over 80 investigational ADCs, and nearly 200 clinical trials and is gaining momentum as an effective approach for targeting cancer.

The new panel provides for customizable ADC content to address complex questions critical for the success of Antibody Drug Conjugates throughout discovery, pre-clinical and clinical development. The panel can be used to directly profile 770 genes addressing essential biological questions relevant to each step in the ADC development workflow, including tumor targeting and antigen expression; ADC internalization; payload release; drug mechanisms of action; target cell death; immunogenic cell death; and mechanisms of resistance.

"With this panel, researchers have a powerful, cutting-edge tool that addresses biological function with deep molecular characterization, expanding insights gained from traditional endpoint assays," said Joseph Beechem, Chief Scientific Officer at NanoString. "The specific and sophisticated characterization will allow us to fully understand mechanisms of action, potential resistance, as well as the role of the immune response."

To learn more about how NanoString is addressing the challenges within the field of ADC, visit NanoString at the virtual World ADC Conference Oct. 11-14. On Oct. 12, NanoString will present "Optimizing ADC Development and Patient-Treatment Selection," led by Dr. Funda Meric-Bernstam, the Chair of the Department of Investigational Cancer Therapeutics, Division of Cancer Medicine, MD Anderson Cancer Center.

On October 12, 2021 Synlogic, Inc. (Nasdaq: SYBX), a clinical stage company bringing the transformative potential of synthetic biology to medicine, reported the publication in Nature of preclinical research with live biotherapeutic products designed using the Company’s Synthetic Biotic platform (Press release, Synlogic, OCT 12, 2021, View Source [SID1234591151]). In the study, a live biotherapeutic product modulated the tumor microenvironment and increased susceptibility to immunotherapy in a murine model. The research was led by Synlogic collaborators and Professor Roger Geiger of the Institute of Oncology Research, Università della Svizzera Italiana, Bellinzona, Switzerland.

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The paper, "Metabolic modulation of tumours with engineered bacteria for immunotherapy" demonstrated that, following intratumoral injection in a murine model, a live biotherapeutic Escherichia coli Nissle 1917 strain engineered to convert ammonia to L-arginine colonized and was active within the tumor microenvironment. Administration of this strain also resulted in increased numbers of tumor-infiltrating T cells and demonstrated synergistic anti-tumor activity when administered in conjunction with anti-PD-L1 immunotherapy.

It has been reported that low intratumoral levels of L-arginine in human cancers may contribute to an ineffective response to immunotherapy. The administration of live biotherapeutics has the potential to improve therapeutic response.

"We were very pleased to collaborate with Professor Geiger on this research and gratified to see a novel Synthetic Biotic approach published in Nature. The data demonstrate another potential method by which our therapeutic platform may be used to modulate underlying biology of relevance to human disease," said David Hava, Ph.D. Chief Scientific Officer at Synlogic. "We believe that our investigational live biotherapeutic approach holds great promise for the development of transformative therapeutics for a variety of serious diseases. We intend to steadfastly focus on our ongoing clinical programs in metabolic diseases, while also supporting the exploration of novel applications for our platform with academic leaders such as Dr. Geiger."

On October 12, 2021 Signify Health, Inc. (NYSE: SGFY), a leading value-based healthcare platform enabled by advanced analytics, technology and nationwide healthcare networks, reported that it will release its financial results for the third quarter 2021 after the market closes on Tuesday, November 9, 2021, and will hold a conference call at 8:30am ET on Wednesday, November 10, 2021 to discuss the results (Press release, Signify Health, OCT 12, 2021, View Source [SID1234591150]).

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Pre-registration is required for participation in the conference call. Please follow the link below to pre-register. After registering, you will be provided with your access details via email.

www.incommuk.com/customers/signifyhealthquarterthree2021

A webcast of the conference call will also be available live on the investor relations section of Signify Health’s website at View Source Please go to the website at least 15 minutes prior to the call to complete the registration process.

The webcast replay will be available through January 10, 2022 on Signify Health’s website at

View Source

On October 12, 2021 PerkinElmer, Inc. (NYSE: PKI), a global leader committed to innovating for a healthier world, reported that the Company will release its third quarter 2021 financial results after market close on Tuesday, November 2, 2021 (Press release, PerkinElmer, OCT 12, 2021, View Source [SID1234591145]). The Company will host a conference call the same day at 5:00 p.m. ET to discuss these results. Prahlad Singh, president and chief executive officer, and Jamey Mock, senior vice president and chief financial officer, will host the conference call.

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To access the call, a live audio webcast of the call will be available via this registration form or on the Investors section of the Company’s website at www.perkinelmer.com.

A replay of the webcast will be available beginning at 7:00 p.m. ET, Tuesday, November 2, 2021 through the Investors section of the Company’s website.

On October 12, 2021 CRISPR Therapeutics (Nasdaq: CRSP), a biopharmaceutical company focused on creating transformative gene-based medicines for serious diseases, reported updated results from the Company’s ongoing Phase 1 CARBON trial evaluating the safety and efficacy of CTX110, its wholly-owned allogeneic CAR-T cell therapy targeting CD19+ B-cell malignancies (Press release, CRISPR Therapeutics, OCT 12, 2021, View Source [SID1234591138]).

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"We are excited to share positive data from our CARBON trial, which show that CTX110 could offer patients with large B-cell lymphomas an immediately available ‘off-the-shelf’ therapy with efficacy similar to autologous CAR-T and a differentiated safety profile," said Samarth Kulkarni, Ph.D., Chief Executive Officer of CRISPR Therapeutics. "Furthermore, we have the potential to improve upon already observed efficacy with a consolidation dosing strategy. Based on these encouraging results, we are planning to expand CARBON into a potentially registrational trial in the first quarter of 2022."

CARBON Trial Overview
The Phase 1 CARBON trial is an open-label, multicenter clinical trial evaluating the safety and efficacy of CTX110 in adult patients with relapsed or refractory B-cell CD19+ malignancies who have received at least two prior lines of therapy. To date, enrollment has been focused on patients with the most aggressive disease presentations, including diffuse large B-cell lymphoma (DLBCL), not otherwise specified (NOS), high-grade double- or triple-hit lymphomas, and transformed follicular lymphoma. The majority of patients had Stage IV lymphoma and were refractory to their last line of therapy before entering the trial. Nine patients received prior autologous stem cell transplant. Patients who received prior autologous CAR-T therapy were not eligible.

As of the August 26, 2021 data cutoff, 30 patients with large B-cell lymphoma (LBCL) had been enrolled, of which 26 patients had received CTX110 with at least 28 days of follow-up and are included in the analysis. Only one enrolled patient did not receive CTX110. Three patients at the time of the data cut had less than 28 days of follow-up and were not evaluable for this analysis.

Patients were infused with a single CTX110 infusion following three days of a standard lymphodepletion regimen consisting of fludarabine (30mg/m2/day) and cyclophosphamide (500mg/m2/day). Patients could be re-dosed with CTX110 following disease progression. The primary endpoints include safety as measured by the incidence of dose limiting toxicities (DLTs) and overall response rate (ORR). Key secondary endpoints include complete response (CR) rate, duration of response and overall survival.

Additional details may be found at clinicaltrials.gov, using identifier: NCT04035434.

Safety
CTX110 was well tolerated across all dose levels. The adverse events of interest for all evaluable patients are shown in the table below.

There were no cases of Graft versus Host Disease (GvHD) and no infusion reactions to either lymphodepleting chemotherapy or CTX110.

All cases of cytokine release syndrome (CRS) were Grade 1 or 2 per the American Society for Transplantation and Cellular Therapy (ASTCT) criteria and either required no specific intervention or resolved following standard CRS management. Neither the frequency nor severity of CRS has increased in patients who were re-dosed with CTX110.

The only case of Grade 3 or higher immune effector cell-associated neurotoxicity syndrome (ICANS) was in the patient with concurrent HHV-6 encephalitis who was previously disclosed. There have been no cases of ICANS in any other patients treated at Dose Level (DL3) through Dose Level (DL4).

Only two patients experienced Grade 3 or higher infections: the previously discussed patient with HHV-6 encephalitis, and one patient who developed pseudomonal sepsis that resolved in four days.

Adverse events of interest N (%)

DL1 (N=3)

DL2 (N=3)

DL3 (N=6)

DL3.5 (N=6)

DL4 (N=8)

DL2+ (N=23)

Gr 1-2

Gr 3+

Gr 1-2

Gr 3+

Gr 1-2

Gr 3+

Gr 1-2

Gr 3+

Gr 1-2

Gr 3+

Gr 1-2

Gr 3+

CRS

1

–

2

–

2

–

3

–

6

–

13

–

(33)

(67)

(33)

(50)

(75)

(57)

ICANS

–

–

1

–

–

–

–

–

–

1

1

1

(33)

(13)

(4)

(4)

GvHD

–

–

–

–

–

–

–

–

–

–

–

–

Infusion reactions

–

–

–

–

–

–

–

–

–

–

–

–

Infections1

–

1

–

–

1

1

1

–

1

1

3

2

(33)

(17)

(17)

(17)

(13)

(13)

(13)

(9)

CRS and ICANS graded per ASTCT criteria; other adverse events graded per CTCAE; (1) All infections (bacterial, fungal, and viral) included

The emerging safety profile of CTX110 is positively differentiated from autologous CAR-T therapies that show high frequencies of severe CRS and ICANS, and from other allogeneic CAR-T therapies that require more toxic lymphodepletion regimens and can result in prolonged immunosuppression and increased risk of serious infections.

Clinical Activity
Data are shown below for the 26 patients that received CTX110 and had at least 28 days of follow-up. The ORR and CR rates for patients treated at DL2 and above are shown both on an intent-to-treat (ITT) and modified ITT (mITT) basis. ITT includes all enrolled patients (n=24 at DL2 and above) whereas mITT includes only those patients who received an infusion of CTX110 (n=23 at DL2 and above). Dose-dependent responses and durable complete responses were seen with CTX110. Disease assessment was performed by investigator review according to the 2014 Lugano response criteria.

Cell dose

DL1

DL2

DL3

DL3.5

DL4

DL2+ mITT

DL2+

(CAR+ T cells)

30×106

100×106

300×106

450×106

600×106

N=23

ITT

N=3

N=3

N=6

N=6

N=8

N=24

Overall response rate (ORR), N (%)

0 (0%)

1 (33%)

3 (50%)

4 (67%)

6 (75%)

14 (61%)

14 (58%)

Complete response (CR) rate, N (%)

0 (0%)

1 (33%)

2 (33%)

3 (50%)

3 (38%)

9 (39%)

9 (38%)

A single dose of CTX110 at DL2 and above resulted in a 58% ORR and 38% CR rate on an ITT basis.
Responses were seen in a variety of patients, including patients who had refractory disease, bulky disease, or who had progressed after prior autologous stem cell transplant.
The data demonstrate the potential for CTX110 to produce durable remissions, as evidenced by a 21% six-month CR rate (4 of the 9 patients who achieved CR at Day 28, remained in CR at 6 months; 5 patients had not reached their 6-month evaluation point), which is in the range of durable remissions observed with approved autologous CAR-T therapies on an ITT basis.
The data provide a strong rationale that consolidation dosing can improve on an already competitive profile for CTX110.
Based on this safety and efficacy profile, the Company plans to expand into a potential registrational trial that incorporates consolidation dosing in Q1 2022. In parallel, the Company continues to advance the rest of its immuno-oncology portfolio and scale its manufacturing capabilities in its new state-of-the-art manufacturing facility in Framingham, Massachusetts.

Conference Call and Webcast
To access the conference call, please dial +1 (866) 952-8559 (domestic) or +1 (785) 424-1743 (international) and reference the conference ID "CRISPR."

A live webcast of the event will be available on the "Events & Presentations" page in the Investors section of the Company’s website at View Source A webcast replay will be available on the CRISPR Therapeutics website after the event and will be archived for 14 days.

About CTX110
CTX110, a wholly owned program of CRISPR Therapeutics, is a healthy donor-derived gene-edited allogeneic CAR-T investigational therapy targeting Cluster of Differentiation 19, or CD19. CTX110 is being investigated in the ongoing CARBON trial.

About CARBON
The ongoing Phase 1 single-arm, multi-center, open label clinical trial, CARBON, is designed to assess the safety and efficacy of several dose levels of CTX110 for the treatment of relapsed or refractory B-cell malignancies.