Q4 2025 Nautilus Biotechnology Inc Earnings Call

February 26, 2026

Operator: Good day, and thank you for standing by. Welcome to the Nautilus Biotechnology Q4 2025 Earnings Conference Call. At this time, all participants are in a listen-only mode. After the speaker's presentation, there will be a question-and-answer session. To ask a question during the session, you will need to press star one one on your telephone. You will then hear an automated message advising your hand is raised. To withdraw your question, please press star one one again. Please be advised that today's conference is being recorded. I would now like to hand the conference over to your first speaker today, Jian Yi, Investor Relations. Please go ahead.

Speaker #1: Good day, and thank you for standing by. Welcome to the Nautilus Biotechnology, Q4, 2025 earnings conference call. At this time, all participants are in a listen-only mode.

Speaker #1: After the speakers' presentation, there will be a question-and-answer session. To ask a question during the session, you will need to press star 11 on your telephone; you will then hear an automated message advising your hand is raised.

Operator: You will then hear an automated message advising your hand is raised. To withdraw your question, please press star one one again. Please be advised that today's conference is being recorded. I would now like to hand the conference over to your first speaker today, Ji-Yon Yi, Investor Relations. Please go ahead.

Speaker #1: To withdraw your question, please press star 11 again. Please be advised that today's conference is being recorded. I would now like to hand the conference over to your first speaker today, Ji-Yon Yi, Investor Relations.

Speaker #1: Please go ahead.

Speaker #2: Thank you. Earlier today, Nautilus released financial results for the quarter ended December 31, 2025. If you haven't received this news release, or if you'd like to be added to the company's distribution list, please send an email to investorrelations@nautilus.bio.

Ji-Yon Yi: Thank you. Earlier today, Nautilus released financial results for Q4 ended 31 December 2025. If you haven't received this news release or if you'd like to be added to the company's distribution list, please send an email to investorrelations@nautilus.bio. Joining me today from Nautilus are Sujal Patel, Co-founder and CEO, Parag Mallick, Co-founder and Chief Scientist, and Anna Mowry, Chief Financial Officer. Before we begin, I'd like to remind you that management will make statements during this call that are forward-looking within the meaning of the federal securities laws. These statements involve material risks and uncertainties that could cause actual results or events to materially differ from those anticipated. Additional information regarding these risks and uncertainties appears in the section entitled Forward-Looking Statements in the press release Nautilus issued today.

Speaker #2: Joining me today from Nautilus are Sujal Patel, co-founder and CEO; Parag Mallick, co-founder and chief scientist; and Anna Mowry, chief financial officer. Before we begin, I'd like to remind you that management will make statements during this call that are forward-looking within the meaning of the Federal Securities Laws.

Speaker #2: These statements involve material risks and uncertainties that could cause actual results or events to materially differ from those anticipated. Additional information regarding these risks and uncertainties appears in the section entitled "Forward-looking Statements" in the press release Nautilus issued today.

Ji-Yon Yi: These statements involve material risks and uncertainties that could cause actual results or events to materially differ from those anticipated. Additional information regarding these risks and uncertainties appears in the section entitled Forward-Looking Statements in the press release Nautilus issued today. Except as required by law, Nautilus disclaims any intention or obligation to update or revise any financial or product pipeline projections or other forward-looking statements, whether because of new information, future events, or otherwise. This conference call contains time-sensitive information and is accurate only as of the live broadcast on 26 February 2026. With that, I'll turn the call over to Sujal.

Speaker #2: Except as required by law, Nautilus disclaims any intention or obligation to update or revise any financial or product pipeline projections or other forward-looking statements whether because of new information, future events, or otherwise.

Ji-Yon Yi: Except as required by law, Nautilus disclaims any intention or obligation to update or revise any financial or product pipeline projections or other forward-looking statements, whether because of new information, future events, or otherwise. This conference call contains time-sensitive information and is accurate only as of the live broadcast on 26 February 2026. With that, I'll turn the call over to Sujal.

Speaker #2: This conference call contains time-sensitive information, and is accurate only as of the live broadcast on February 26, 2026. With that, I'll turn the call over to Sujal.

Speaker #3: Thanks, John, and thank you all for joining us today. Before turning to the quarter, I want to briefly remind everyone of what we're building and why we believe it matters.

Sujal Patel: Thanks, Jian, and thank you all for joining us today. Before turning to the quarter, I want to briefly remind everyone of what we're building and why we believe it matters. Nautilus was founded to address a long-standing challenge in life sciences, the lack of technologies capable of comprehensively measuring the proteome with the sensitivity, scale, and reproducibility needed to fully understand biology and disease. Our proprietary Iterative Mapping methodology is designed to analyze single, intact protein molecules at scale and generate highly reproducible digital protein counts. This methodology is delivered through the Nautilus platform, an integrated system of instrumentation, consumables, and software, which can support both broad-scale proteome analysis and targeted proteoform characterization on a single platform.

Speaker #3: Nautilus was founded to address a long-standing challenge in life sciences: the lack of technologies capable of comprehensively measuring the proteome with the sensitivity, scale, and reproducibility needed to fully understand biology and disease.

Speaker #3: Our proprietary iterative mapping methodology is designed to analyze single intact protein molecules at scale, and generate highly reproducible digital protein counts. This methodology is delivered through the Nautilus platform, an integrated system of instrumentation, consumables, and software, which can support both broad-scale proteome analysis and targeted proteoform characterization on a single platform.

Sujal Patel: Our proprietary Iterative Mapping methodology is designed to analyze single, intact protein molecules at scale and generate highly reproducible digital protein counts. This methodology is delivered through the Nautilus platform, an integrated system of instrumentation, consumables, and software, which can support both broad-scale proteome analysis and targeted proteoform characterization on a single platform.

Speaker #3: Over time, we believe this data foundation will unlock new biological insight, integrate more effectively with other omics modalities, support next-generation AI-driven discovery in human health and medicine, and ultimately help accelerate the development of new therapeutics and diagnostics.

Sujal Patel: Over time, we believe this data foundation will unlock new biological insight, integrate more effectively with other omics modalities, support next-generation AI-driven discovery in human health and medicine, and ultimately help accelerate the development of new therapeutics and diagnostics. With that context, Q4 marked a strong close to 2025 as we continued to make tangible progress toward commercialization, deepen external validation, and build momentum with leading research institutions. A key highlight of that progress was our presence at the US Human Proteome Organization Conference, or US HUPO, in St. Louis, Missouri this week, where we publicly unveiled the Nautilus Voyager instrument in dramatic fashion to a large audience of influential researchers and prospective future customers, providing the proteomics community with its first tangible view of the instrument we've been building.

Speaker #3: With that context, Q4 marked a strong close to 2025 as we continue to make tangible progress toward commercialization, deepen external validation, and build momentum with leading research institutions.

Sujal Patel: A key highlight of that progress was our presence at the US Human Proteome Organization Conference, or US HUPO, in St. Louis, Missouri this week, where we publicly unveiled the Nautilus Voyager instrument in dramatic fashion to a large audience of influential researchers and prospective future customers, providing the proteomics community with its first tangible view of the instrument we've been building.

Speaker #3: A key highlight of that progress was our presence at the U.S. Human Proteome Organization conference, or U.S. HUPO, in St. Louis, Missouri this week.

Speaker #3: Where we publicly unveiled the Nautilus Voyager instrument in dramatic fashion to a large audience of influential researchers and prospective future customers, providing the proteomics community with its first tangible view of the instrument we've been building.

Speaker #3: The response was highly positive and reinforced the strong interest we're seeing from researchers seeking a new class of protein measurement technology. Importantly, when designing Voyager, we were intentional about creating an instrument that looked and felt different, one that conveyed sophistication and innovation while still being approachable and easy to use.

Sujal Patel: The response was highly positive and reinforced the strong interest we're seeing from researchers seeking a new class of protein measurement technology. Importantly, when designing Voyager, we were intentional about creating an instrument that looked and felt different, one that conveyed sophistication and innovation while still being approachable and easy to use. We wanted an instrument that reflected the ambition of what we're building, while also fitting naturally into modern research environments. The feedback we received confirmed that this balance resonated strongly with the community. Building on the capabilities of the Voyager instrument and supported by the encouraging tau data we've seen emerging from our early collaborators, we elected to launch our early access program for Iterative Mapping in January, earlier than previously communicated.

Speaker #3: We wanted an instrument that reflected the ambition of what we're building. While also fitting naturally into modern research environments. And the feedback we received confirmed that this balance resonated strongly with the community.

Sujal Patel: The feedback we received confirmed that this balance resonated strongly with the community. Building on the capabilities of the Voyager instrument and supported by the encouraging tau data we've seen emerging from our early collaborators, we elected to launch our early access program for Iterative Mapping in January, earlier than previously communicated.

Speaker #3: Building on the capabilities of the Voyager instrument and supported by the encouraging tau data we've seen emerging from our early collaborators, we elected to launch our early access program for iterative mapping in January, earlier than previously communicated.

Speaker #3: This milestone represents a meaningful step in Nautilus' transition from development to active customer engagement, enabling partners to submit samples, receive data, and provide feedback in a streamlined manner.

Sujal Patel: This milestone represents a meaningful step in Nautilus's transition from development to active customer engagement, enabling partners to submit samples, receive data, and provide feedback in a streamlined manner. Initial customer response has been encouraging, while these early engagements are not intended to drive near-term revenue, they are designed to enable real biological discovery, support publications and grant applications, and ensure our workflows and data outputs align closely with customers' needs, an approach consistent with how many transformative life sciences platforms have successfully entered the market. The early access program will begin with our tau proteoform assay and establish a foundation for future assay expansion, covering additional proteoform targets and broad-scale applications. Importantly, we believe this early access launch also reflects a forthcoming diversity of assays for our platform beyond tau. For example, in late January, we announced a collaboration with Weill Cornell Medicine-Qatar and the Michael J.

Speaker #3: Initial customer response has been encouraging, and while these early engagements are not intended to drive near-term revenue, they are designed to enable real biological discovery, support publications, and grant applications, and ensure our workflows and data outputs align closely with customers' needs.

Speaker #3: An approach consistent with how many transformative life sciences platforms have successfully entered the market. The early access program will begin with our tau proteoform assay and establish a foundation for future assay expansion covering additional proteoform targets and broad-scale applications.

Sujal Patel: The early access program will begin with our tau proteoform assay and establish a foundation for future assay expansion, covering additional proteoform targets and broad-scale applications. Importantly, we believe this early access launch also reflects a forthcoming diversity of assays for our platform beyond tau. For example, in late January, we announced a collaboration with Weill Cornell Medicine-Qatar and the Michael J. Fox Foundation, focused on alpha-synuclein proteoforms in Parkinson's disease.

Speaker #3: Importantly, we believe this early access launch also reflects a forthcoming diversity of assays for our platform beyond tau. For example, in late January, we announced a collaboration with Weill Cornell Medicine-Qatar and the Michael J.

Speaker #3: Fox Foundation focused on alpha-synuclein proteoforms in Parkinson's disease. This MJFF-funded project, $1.6 million in total, with $1.2 million coming to Nautilus, combines Professor Hilal Lashua's deep expertise in neurodegeneration with Nautilus' ability to measure proteins and their functional variants at the single molecule resolution.

Sujal Patel: Fox Foundation, focused on alpha-synuclein proteoforms in Parkinson's disease. This MJFF-funded project, $1.6 million in total, with $1.2 million coming to Nautilus, combines Professor Hilal Lashuel's deep expertise in neurodegeneration with Nautilus's ability to measure proteins and their functional variants at the single-molecule resolution. Understanding alpha-synuclein proteoforms is a priority for MJFF, and we believe this collaboration is a strong example of how Iterative Mapping can be extended to additional high-value proteoform targets and disease areas over time. On the technology front, we continued to make strong progress as we moved into the later stages of our broad-scale assay configuration change. This work is designed to better align with our expanding probe library and improve overall platform performance. We're now seeing the first data from the updated assay on new chips, and early readouts are encouraging.

Sujal Patel: This MJFF-funded project, $1.6 million in total, with $1.2 million coming to Nautilus, combines Professor Hilal Lashuel's deep expertise in neurodegeneration with Nautilus's ability to measure proteins and their functional variants at the single-molecule resolution. Understanding alpha-synuclein proteoforms is a priority for MJFF, and we believe this collaboration is a strong example of how Iterative Mapping can be extended to additional high-value proteoform targets and disease areas over time.

Speaker #3: Understanding alpha-synuclein proteoforms is a priority for MJFF, and we believe this collaboration is a strong example of how iterative mapping can be extended to additional high-value proteoform targets and disease areas over time.

Sujal Patel: On the technology front, we continued to make strong progress as we moved into the later stages of our broad-scale assay configuration change. This work is designed to better align with our expanding probe library and improve overall platform performance. We're now seeing the first data from the updated assay on new chips, and early readouts are encouraging.

Speaker #3: On the technology front, we continue to make strong progress as we moved into the later stages of our broad-scale assay configuration change. This work is designed to better align with our expanding probe library and improve overall platform performance.

Speaker #3: We're now seeing the first data from the updated assay on new chips and early readouts are these technical details in more depth, and I'll return later to discuss how this progress informs our expectations for 2026.

Sujal Patel: Parag will walk through these technical details in more depth, and I'll return later to discuss how this progress informs our expectations for 2026. Taken together, these developments reflect steady progress towards commercialization, grounded in real samples, real data, real customer engagement, and increasing external validation. Throughout 2025, we remained disciplined in how we invested our resources, meaningfully reducing expenses while continuing to advance our most important technical and strategic priorities. I want to recognize our scientific and engineering teams for their continued focus and execution. With that, I'll turn the call over to Parag.

Speaker #3: Taken together, these developments reflect steady progress towards commercialization, grounded in real samples, real data, real customer engagement, and increasing external validation. Throughout 2025, we remain disciplined in how we invested our resources meaningfully reducing expenses while continuing to advance our most important technical and strategic priorities.

Sujal Patel: Throughout 2025, we remained disciplined in how we invested our resources, meaningfully reducing expenses while continuing to advance our most important technical and strategic priorities. I want to recognize our scientific and engineering teams for their continued focus and execution. With that, I'll turn the call over to Parag.

Speaker #3: I want to recognize our scientific and engineering teams for their continued focus and execution. With that, I'll turn the call over to Parag.

Speaker #4: Thanks, Sujal. I'll now provide an update on our technology and product progress, including what we're learning from our development work and the external validation we're seeing through collaborations.

Parag Mallick: Thanks, Sujal. I'll now provide an update on our technology and product progress, including what we're learning from our development work and the external validation we're seeing through collaborations. Overall, Q4 was a strong quarter of execution for our product and scientific teams. We continue to see growing validation of the Nautilus platform through both internal development and external partnerships. Importantly, we are increasingly moving beyond demonstrating that the technology works and towards applying it to obtain remarkable biological insights not possible with existing proteomics approaches. This shift from capability to meaningful application is an important marker of platform maturity and a central focus for the team. Collaborations continue to play a critical role in validating the platform and demonstrating real-world relevance.

Speaker #4: Overall, Q4 was a strong quarter of execution for our product and scientific teams. We continue to see growing validation of the Nautilus platform through both internal development and external partnerships.

Parag Mallick: Importantly, we are increasingly moving beyond demonstrating that the technology works and towards applying it to obtain remarkable biological insights not possible with existing proteomics approaches. This shift from capability to meaningful application is an important marker of platform maturity and a central focus for the team. Collaborations continue to play a critical role in validating the platform and demonstrating real-world relevance.

Speaker #4: Importantly, we are increasingly moving beyond demonstrating that the technology works and towards applying it to obtain remarkable biological insights not possible with existing proteomics approaches.

Speaker #4: This shift from capability to meaningful application is an important marker of platform maturity and a central focus for the team. Collaborations continue to play a critical role in validating the platform and demonstrating real-world relevance.

Speaker #4: During the quarter, we completed work with the Buck Institute for Research on Aging, culminating in the presentation of novel tau biology at World HUPO, and most recently, at U.S.

Parag Mallick: During the quarter, we completed work with the Buck Institute for Research on Aging, culminating in the presentation of novel tau biology at World HUPO, and most recently at US HUPO, and we are now supporting our partners as they prepare their findings for publication. In parallel, through our collaboration with the Allen Institute for Brain Science, we analyzed human brain samples spanning multiple brain regions, genetic backgrounds, and disease severities. We believe this work represents the most comprehensive and quantitative tau proteoform landscape study to date. Notably, we are observing clear differences in tau proteoform patterns across disease severity and brain regions, signals that are not detectable using conventional proteomics approaches, and that may help explain variability in disease progression and clinical outcomes. We also anticipate that such insights may be essential for developing the next generation of therapies for neurodegenerative diseases.

Speaker #4: HUPO, and we are now supporting our partners as they prepare their findings for publication. In parallel, through our collaboration with the Allen Institute for Brain Science, we analyzed human brain samples spanning multiple brain regions: genetic backgrounds and disease severities.

Speaker #4: We believe this work represents the most comprehensive and quantitative tau proteoform landscape study to date. Notably, we are observing clear differences in tau proteoform patterns across disease severity and brain regions.

Parag Mallick: Notably, we are observing clear differences in tau proteoform patterns across disease severity and brain regions, signals that are not detectable using conventional proteomics approaches, and that may help explain variability in disease progression and clinical outcomes. We also anticipate that such insights may be essential for developing the next generation of therapies for neurodegenerative diseases.

Speaker #4: Signals that are not detectable using conventional proteomics approaches and that may help explain variability in disease progression and clinical outcomes. We also anticipate that such insights may be essential for developing the next generation of therapies for neurodegenerative diseases.

Speaker #4: Stepping back, what stands out is that the data emerging from these collaborations is not only technically robust but biologically compelling. With each additional study, we gain confidence that iterative mapping is enabling access to important biology that has remained out of reach, for existing technologies.

Parag Mallick: Stepping back, what stands out is that the data emerging from these collaborations is not only technically robust, but biologically compelling. With each additional study, we gain confidence that Iterative Mapping is enabling access to important biology that has remained out of reach for existing technologies. We believe this new class of proteoform-level data has the potential to drive real-world impact by deepening our understanding of disease mechanisms, revealing new therapeutic targets, and enabling the development of more precise biomarkers for diagnosis, patient stratification, and treatment monitoring. Ultimately, our goal is to demonstrate to the broader scientific community that this represents a transformative foundation of information, one that can help accelerate drug discovery workflows and improve the probability of success in developing new therapeutics. From a platform development perspective, we made meaningful progress across both our broad-scale assay and our proteoform assay portfolio.

Speaker #4: We believe this new class of proteoform-level data has the potential to drive real-world impact by deepening our understanding of disease mechanisms, revealing new therapeutic targets, and enabling the development of more precise biomarkers for diagnosis, patient stratification, and treatment monitoring.

Speaker #4: Ultimately, our goal is to demonstrate to the broader scientific community that this represents a transformative foundation of information, one that can help accelerate drug discovery workflows and improve the probability of success in developing new therapeutics.

Parag Mallick: Ultimately, our goal is to demonstrate to the broader scientific community that this represents a transformative foundation of information, one that can help accelerate drug discovery workflows and improve the probability of success in developing new therapeutics. From a platform development perspective, we made meaningful progress across both our broad-scale assay and our proteoform assay portfolio.

Speaker #4: From a platform development perspective, we made meaningful progress across both our broad-scale assay and our proteoform assay portfolio. While also gaining greater clarity on the remaining work required to reach our next milestones.

Parag Mallick: while also gaining greater clarity on the remaining work required to reach our next milestones. Starting with the broad scale assay, we continued advancing our assay, including advancing the assay configuration change we have discussed previously, and are now routinely employing our new configuration. During the quarter, we achieved several encouraging milestones, including performing our largest scale experiments to date, which demonstrated Iterative Mapping-based decoding of proteins from increasingly complex mixtures, including cell lysates. In addition, we made good progress on hardening the fabrication process for our new flow cell configuration and showing assay performance characteristics, such as increased on-target binding, that give us indications our new assay configuration will enable an expanded affinity reagent library. The work completed in Q4 helped validate key elements of the new configuration and clarified the primary levers needed to drive further performance improvements as we scale towards complex biological samples.

Speaker #4: Starting with the broad-scale assay, we continue to advancing our assay, including advancing the assay configuration change we have discussed previously and are now routinely employing our new configuration.

Speaker #4: During the quarter, we achieved several encouraging milestones, including performing our largest-scale experiments to date. Which demonstrated iterative mapping-based decoding, a proteins from increasingly complex mixtures, including cell lysates.

Speaker #4: In addition, we made good progress on hardening the fabrication process for our new flow cell configuration. And showing assay performance characteristics, such as increased on-target binding, that give us indications our new assay configuration will enable an expanded affinity reagent library.

Parag Mallick: In addition, we made good progress on hardening the fabrication process for our new flow cell configuration and showing assay performance characteristics, such as increased on-target binding, that give us indications our new assay configuration will enable an expanded affinity reagent library. The work completed in Q4 helped validate key elements of the new configuration and clarified the primary levers needed to drive further performance improvements as we scale towards complex biological samples.

Speaker #4: The work completed in Q4 helped validate key elements of the new configuration and clarified the primary levers needed to drive further performance improvements as we scale towards complex biological samples.

Speaker #4: Progress on proteoform assays remains strong. The tau proteoform assay continues to track as our first early access offering and we remain on schedule to begin processing samples through the early access program by the end of Q1.

Parag Mallick: Progress on proteoform assays remains strong. The tau proteoform assay continues to track as our first early access offering, and we remain on schedule to begin processing samples through the early access program by the end of Q1. Verification and validation activities are largely complete, and the assay is meeting our requirements for accuracy, dynamic range, reproducibility, and stability, marking an important step as we transition tau from development into a high-quality, commercial-ready product. In parallel, we formally initiated our proteoform expansion pipeline. As Sujal mentioned, we launched an 18-month collaboration funded by The Michael J. Fox Foundation to develop an alpha-synuclein proteoform quantification assay, extending the platform into Parkinson's disease. This program includes development of a pilot assay focused on key post-translational modifications, optimization of enrichment and sample preparation workflows, and application of the technology to human brain and biofluid samples.

Speaker #4: Verification and validation activities are largely complete and the assay is meeting our requirements for accuracy, dynamic range, reproducibility, and stability. Marking an important step as we transition tau from development into a high-quality commercial-ready product.

Speaker #4: In parallel, we formally initiated our proteoform expansion pipeline. As Sujal mentioned, we launched an 18-month collaboration funded by the Michael J. Fox Foundation to develop an alpha-synuclein proteoform quantification assay.

Parag Mallick: As Sujal mentioned, we launched an 18-month collaboration funded by The Michael J. Fox Foundation to develop an alpha-synuclein proteoform quantification assay, extending the platform into Parkinson's disease. This program includes development of a pilot assay focused on key post-translational modifications, optimization of enrichment and sample preparation workflows, and application of the technology to human brain and biofluid samples.

Speaker #4: Extending the platform into Parkinson's disease. This program includes development of a pilot assay focused on key post-translational modifications, optimization of enrichment and sample preparation workflows, and application of the technology to human brain and biofluid samples.

Speaker #4: We view this collaboration as an important opportunity to further demonstrate the breadth of iterative mapping beyond tau and to expand our proteoform capabilities into additional high-value disease targets.

Parag Mallick: We view this collaboration as an important opportunity to further demonstrate the breadth of Iterative Mapping beyond tau and to expand our proteoform capabilities into additional high-value disease targets. While much of our current momentum is in neurodegeneration, it's important to emphasize that Iterative Mapping is not limited to neuroscience. We see meaningful long-term potential across oncology, immunology, cardiology, and beyond. We are currently evaluating multiple oncology-focused candidate proteins with the goal of having an oncology-focused proteoform assay enter early access in the second half of 2026. We believe oncology represents a compelling next market opportunity, providing access to a broader customer base, while also aligning well with the capabilities of our platform to deliver proteoform-level resolution and highly reproducible measurement in complex biological systems. Overall, Q4 represented a strong quarter of technical execution as we continued advancing our Voyager instrument and end-to-end platform.

Speaker #4: While much of our current momentum is in neurodegeneration, it's important to emphasize that iterative mapping is not limited to neuroscience. We see meaningful long-term potential across oncology, immunology, cardiology, and beyond.

Speaker #4: We are currently evaluating multiple oncology-focused candidate proteins with the goal of having an oncology-focused proteoform assay enter early access in the second half of 2026.

Parag Mallick: We believe oncology represents a compelling next market opportunity, providing access to a broader customer base, while also aligning well with the capabilities of our platform to deliver proteoform-level resolution and highly reproducible measurement in complex biological systems. Overall, Q4 represented a strong quarter of technical execution as we continued advancing our Voyager instrument and end-to-end platform.

Speaker #4: We believe oncology represents a compelling next market opportunity providing access to a broader customer base while also aligning well with the capabilities of our platform to deliver proteoform-level resolution and highly reproducible measurement in complex biological systems.

Speaker #4: Overall, Q4 represented a strong quarter of technical execution as we continued advancing our Voyager instrument and end-to-end platform. We made meaningful progress on the broad-scale assay configuration change and began generating initial data from the new approach, while also advancing our proteoform portfolio, with tau on track for early access sample processing by the end of this quarter.

Parag Mallick: We made meaningful progress on the broad scale assay configuration change and began generating initial data from the new approach, while also advancing our proteoform portfolio, with tau on track for early access sample processing by the end of this quarter. At the same time, the growing body of externally generated data from collaborators like the Buck Institute and the Allen Institute continues to validate both the robustness of our measurements and the unique biological insight enabled by Iterative Mapping. Taken together, these developments reflect continued platform maturation and reinforce our confidence in the technical foundation required to scale our assays, broaden our target portfolio, and support future commercial deployment. With that, I'll turn the call over to Anna to review our financials.

Speaker #4: At the same time, the growing body of externally generated data from collaborators like the Buck Institute and the Allen Institute continues to validate both the robustness of our measurements and the unique biological insight enabled by iterative mapping.

Speaker #4: Taken together, these developments reflect continued platform maturation and reinforce our confidence in the technical foundation required to scale our assays broaden our target portfolio and support future commercial deployment.

Parag Mallick: Taken together, these developments reflect continued platform maturation and reinforce our confidence in the technical foundation required to scale our assays, broaden our target portfolio, and support future commercial deployment. With that, I'll turn the call over to Anna to review our financials.

Speaker #4: With that, I'll turn the call over to Anna to review our financials.

Speaker #3: Thanks, Parag. Turning to our financial results, we continue to demonstrate strong operating discipline in Q4 and throughout 2025. Total operating expenses were $15.4 million for the fourth quarter of 2025, a decrease of 23% from the prior year period, and $66.8 million for the fiscal year 2025, a decrease of 18% year over year.

Anna Mowry: Thanks, Parag. Turning to our financial results, we continued to demonstrate strong operating discipline in Q4 and throughout 2025. Total operating expenses were $15.4 million for Q4 of 2025, a decrease of 23% from the prior year period, and $66.8 million for the fiscal year 2025, a decrease of 18% year-over-year. Research and development expenses were $41.1 million for fiscal year 2025, compared to $50.5 million in fiscal year 2024, representing a decrease of $9.4 million or 19%. This decrease was driven primarily by a $4.5 million reduction in laboratory supplies and equipment expenses, reflecting operating efficiencies, lower development-related costs, and continued cost optimization efforts.

Speaker #3: Research and development expenses were $41.1 million for fiscal year 2025 compared to $50.5 million in fiscal year 2024, representing a decrease of 9.4 million or 19%.

Speaker #3: This decrease was driven primarily by a $4.5 million reduction in laboratory supplies and equipment expenses reflecting operating efficiencies, lower development-related costs, and continued cost optimization efforts.

Speaker #3: We also saw a $2.4 million decrease in salaries and related benefits driven by savings from the reduction in force implemented in the first quarter of 2025 along with a $1.9 million decrease in stock-based compensation expense.

Anna Mowry: We also saw a $2.4 million decrease in salaries and related benefits, driven by savings from the reduction in force implemented in Q1 2025, along with a $1.9 million decrease in stock-based compensation expense. General and administrative expenses were $25.7 million for fiscal year 2025, compared to $31.0 million in fiscal year 2024, a decrease of $5.3 million or 17%. This decrease was primarily due to a $3.9 million reduction in stock-based compensation expense, along with a $1.3 million decrease in professional services, largely attributable to lower legal and consulting costs. We ended Q4 with $156.1 million in cash equivalents, and investments...

Speaker #3: General and administrative expenses were $25.7 million for fiscal year 2025 compared to $31.0 million in fiscal year 2024, a decrease of $5.3 million, or 17%.

Speaker #3: This decrease was primarily due to a $3.9 million reduction in stock-based compensation expense along with a $1.3 million decrease in professional services largely attributable to lower legal and consulting costs.

Speaker #3: We ended the quarter with $156.1 million in cash, cash equivalents, and investments. Cash burn in 2025 was $50.2 million down from $57.8 million in 2024 reflecting the benefit of lower headcount and development expenses.

Anna Mowry: Cash burn in 2025 was $50.2 million, down from $57.8 million in 2024, reflecting the benefit of lower headcount and development expenses. Looking ahead, we expect total operating expenses for the full year 2026 to increase as we continue investing in platform development, support the expansion of our early access program, and advance commercial readiness activities. We currently anticipate total operating expense growth of approximately 15% to 20% in 2026, and we expect full year 2026 cash burn to be in the range of $65 to 70 million. Based on these assumptions, we continue to believe our financial plan supports a cash runway that extends through 2027.

Speaker #3: Looking ahead, we expect total operating expenses for the full year 2026 to increase as we continue investing in platform development, support the expansion of our early access program, and advance commercial readiness activities.

Speaker #3: We currently anticipate total operating expense growth of approximately $15 to 20% in 2026 and we expect full year 2026 cash burn to be in the range of $65 to $70 million.

Speaker #3: Based on these assumptions, we continue to believe our financial plan supports a cash runway that extends through 2027. Following the launch of our early access program in January, our initial customer engagements are primarily with academic key opinion leaders seeking early access to the tau offering to support exploratory research and grant applications.

Anna Mowry: Following the launch of our early access program in January, our initial customer engagements are primarily with academic key opinion leaders seeking early access to the tau offering to support exploratory research and grant applications. While we expect modest services revenue later in 2026, we anticipate the primary revenue ramp will begin in 2027 once we start shipping instruments. As a reminder, instrument placements drive our recurring consumables business, and together they create a scalable top line. We believe the instrument and consumables ramp will accelerate meaningfully once both our Proteoform and broad scale capabilities are generally available, enabling customers to deploy the full power of the platform and driving broader commercial adoption. As Sujal noted earlier, we also announced grant funding from The Michael J. Fox Foundation to support development of an alpha-synuclein proteoform assay.

Speaker #3: While we expect modest services revenue later in 2026, we anticipate the primary revenue ramp will begin in 2027 once we start shipping instruments. As a reminder, instrument placements drive our recurring consumables business and together they create a scalable top line.

Speaker #3: We believe that instrument and consumables ramp will accelerate meaningfully once both our proteoform and broad-scale capabilities are generally available enabling customers to deploy the full power of the platform and driving broader commercial adoption.

Anna Mowry: We believe the instrument and consumables ramp will accelerate meaningfully once both our Proteoform and broad scale capabilities are generally available, enabling customers to deploy the full power of the platform and driving broader commercial adoption. As Sujal noted earlier, we also announced grant funding from The Michael J. Fox Foundation to support development of an alpha-synuclein proteoform assay.

Speaker #3: As Sujal noted earlier, we also announced grant funding from the Michael J. Fox Foundation to support development of an alpha-synuclein proteoform assay. Under this agreement, we expect to receive approximately $1.2 million with development and sample analysis work occurring over approximately 18 months across 2026 and 2027.

Anna Mowry: Under this agreement, we expect to receive approximately $1.2 million, with development and sample analysis work occurring over approximately 18 months across 2026 and 2027. Revenue will be recognized as the underlying work progresses. Back to you, Sujal.

Speaker #3: Revenue will be recognized as the underlying work progresses. Back to you, Sujal.

Speaker #1: Thanks, Anna. As we wrap up, 2025 was a year of meaningful progress for Nautilus as we continue advancing the platform and began transitioning toward external engagement.

Sujal Patel: Thanks, Anna. As we wrap up, 2025 was a year of meaningful progress for Nautilus as we continued advancing the platform and began transitioning toward external engagement. That momentum carried into early 2026 with the launch of our Iterative Mapping early access program and was further highlighted this week by the debut of the Voyager instrument at US HUPO, where we introduced the system directly to the proteomics community. Together, these milestones represent important steps in putting the platform into the hands of researchers. Looking ahead, we expect 2026 to be a pivotal execution year. We plan to begin progressing early access customers into tau services projects, expand early access to include a second proteoform assay focused on an oncology target, and introduce broad scale capabilities into early access later in the year.

Speaker #1: That momentum carried into early 2026 with the launch of our iterative mapping early access program and was further highlighted this week by the debut of the Voyager instrument at USUFO where we introduced the system directly to the proteomics community.

Speaker #1: Together, these milestones represent important steps in putting the platform into the hands of researchers. Looking ahead, we expect 2026 to be a pivotal execution year.

Sujal Patel: Together, these milestones represent important steps in putting the platform into the hands of researchers. Looking ahead, we expect 2026 to be a pivotal execution year. We plan to begin progressing early access customers into tau services projects, expand early access to include a second proteoform assay focused on an oncology target, and introduce broad scale capabilities into early access later in the year.

Speaker #1: We plan to begin progressing early access customers into tau services projects expand early access to include a second proteoform assay focused on an oncology target and introduce broad-scale capabilities into early access later in the year.

Speaker #1: In parallel, we expect to place Voyager instruments externally through beta deployments as an important validation step ahead of commercialization. We expect to initiate our commercial launch in late 2026 by opening the Voyager platform for pre-orders with instrument installations at customer sites beginning in early 2027.

Sujal Patel: In parallel, we expect to place Voyager instruments externally through beta deployments as an important validation step ahead of commercialization. We expect to initiate our commercial launch in late 2026 by opening the Voyager platform for pre-orders, with instrument installations at customer sites beginning in early 2027. At launch, we expect general availability to include the Voyager instrument, our tau proteoform assay, and a second proteoform assay. We anticipate general availability of our broad scale capabilities in the first half of 2027 as we continue expanding our platform's assay portfolio. We're encouraged by the momentum we continue to see from collaborators and partners applying Nautilus's Iterative Mapping technology to complex disease-relevant biology and by the steady progress we've made across our assay development and operational priorities.

Speaker #1: At launch, we expect general availability to include the Voyager instrument, our tau proteoform assay, and a second proteoform assay. We anticipate general availability of our broad-scale capabilities in the first half of 2027 as we continue expanding our platform's assay portfolio.

Sujal Patel: We anticipate general availability of our broad scale capabilities in the first half of 2027 as we continue expanding our platform's assay portfolio. We're encouraged by the momentum we continue to see from collaborators and partners applying Nautilus's Iterative Mapping technology to complex disease-relevant biology and by the steady progress we've made across our assay development and operational priorities.

Speaker #1: We're encouraged by the momentum we continue to see from collaborators and partners applying Nautilus's iterative mapping technology to complex disease-relevant biology and by the steady progress we've made across our assay development and operational priorities.

Speaker #1: Together, these efforts position us to begin translating years of investment in what we believe will be meaningful scientific and ultimately commercial impact. I'm proud of the work that our team has accomplished and grateful to our collaborators for their partnership and trust.

Sujal Patel: Together, these efforts position us to begin translating years of investment in what we believe will be meaningful, scientific, and ultimately commercial impact. I'm proud of the work that our team has accomplished and grateful to our collaborators for their partnership and trust. With a strong foundation in place and a clear path forward, we remain focused on disciplined execution as we advance the platform towards broader deployment. Thank you for joining us today. With that, we'll be happy to take your questions. Operator?

Speaker #1: With a strong foundation in place and a clear path forward, we remain focused on disciplined execution as we advance the platform towards broader deployment.

Speaker #1: Thank you for joining us today. With that, we'll be happy to take your questions.

Speaker #2: Thank you. At this time, we will conduct the question-and-answer session. As a reminder, to ask a question, you will need to press star 11 on your telephone and wait for your name to be announced.

Operator: Thank you. At this time, we will conduct the question-and-answer session. As a reminder, to ask a question, you will need to press star one one on your telephone and wait for your name to be announced. To withdraw your question, please press star one one again. Please stand by. Our first question comes from Subbu Nambi from Guggenheim. Your line is now open.

Speaker #2: To withdraw your question, please press star 11 again. Please stand by. Our first question comes from Subhu Nambi from Guggenheim. Your line is now open.

Subbu Nambi: Hey, guys. Thank you for taking my questions. There was a lot of focus on the technical milestones you achieved in Q4 that provide you with a foundation for further technical improvements. Building off of that, I have a couple questions. What comes next? By that I mean, what are the next milestones, and what metrics materially get better, building off of the technical milestones you achieved in Q4? Second, have you shared these milestones with any of the key customers, especially those focused on tau? If so, have these new developments catalyzed the path to placement? Thank you so much.

Speaker #3: Hey, guys. Thank you for taking my questions. There was a lot of focus on the technical milestones you achieved in Q4 that provide you with a foundation for further technical improvements.

Speaker #3: Building off of that, I have a couple of questions. What comes next by that I mean, what are the next milestones and what metrics, materially, get better building off of the technical milestones you achieved in Q4?

Speaker #3: And second, have you shared these milestones with any of the key customers, especially those focused on tau? And if so, have these new developments catalyzed a path to placements?

Speaker #3: Thank you so much.

Speaker #4: Thanks, Subhu. I'll take that one. I think there are a couple of key sets of technical milestones, and I'll try and describe each of them.

Parag Mallick: Thanks, Subbu. I'll take that one. I think there are a couple key sets of technical milestones, and I'll try and describe each of them. One of the really key technical milestones was the completion of the final studies of the tau proteoform assay to make sure that it was ready and an incredibly performant assay for our early access program. That data has been shared back with early customers. They're excited about the quality of the assay and really thrilled that we're at the data that we're able to produce.

Speaker #4: One of the really key technical milestones was the completion of the final studies of the tau proteoform assay to make sure that it was ready and an incredibly performant assay.

Speaker #4: For our early access program, that data has been shared back with early customers. They're excited about the quality of the assay and really thrilled that we're at the data that we're able to produce.

Parag Mallick: The second set of progress, we're on instrument readiness. As we mentioned, coming out of our evaluation instrument at the Buck, data we learned from that and internally, that was really what positioned us for the announcement of the reveal of the instrument at the US HUPO Conference earlier this week. Tremendous excitement about folks really being able to get their hands on the instrument and see it was great. I think the other aspect that we've been discussing in terms of moving forward are the expansion of the proteoform platform to additional targets. We mentioned alpha-synuclein and an oncology-focused target, and I think the people are remaining very excited about proteoforms across domains.

Speaker #4: The second set of progress were on instrument readiness and, as we mentioned, coming out of our evaluation instrument at the Buck data we learned from that and internally that was really what positioned us for the announcement of the reveal of the instrument at the USUFO conference earlier this week.

Speaker #4: And tremendous excitement about folks really being able to get their hands on the instrument and see it was great. I think the other aspect that we've been discussing in terms of moving forward are the expansion of the proteoform platform to additional targets. We mentioned alpha-synuclein and an oncology-focused target.

Parag Mallick: I think the other aspect that we've been discussing in terms of moving forward are the expansion of the proteoform platform to additional targets. We mentioned alpha-synuclein and an oncology-focused target, and I think the people are remaining very excited about proteoforms across domains. Seeing progress towards other proteoforms, validating that the platform is not just a neuro platform, but is a platform that can apply across different domains, is something that we've heard a lot of positive excitement about.

Speaker #4: And I think the people are remaining very excited about proteoforms across domains. And so seeing progress towards other proteoforms, validating that the platform is not just a neuro platform, but is a platform that can apply across different domains is something that we've heard a lot of positive excitement about.

Parag Mallick: Seeing progress towards other proteoforms, validating that the platform is not just a neuro platform, but is a platform that can apply across different domains, is something that we've heard a lot of positive excitement about. On the broad scale side, as we mentioned, the expansion of both the scale of assays that we're performing, as well as the further progress on the configuration change. I think all of those things are really key contributors. As we look forward, what we're looking at are, you know, levers like increase it, further increasing on-target binding, minimizing off-target binding. We continue to progress working on assay stability of the new configuration chips that are stable over hundreds of cycles. All of these are challenges that require optimization, not innovation.

Speaker #4: And then on the broad-scale side as we mentioned, the expansion of both the scale of assays that we're performing as well as the further progress on the configuration change I think all of those things are really key contributors.

Parag Mallick: On the broad scale side, as we mentioned, the expansion of both the scale of assays that we're performing, as well as the further progress on the configuration change. I think all of those things are really key contributors. As we look forward, what we're looking at are, you know, levers like increase it, further increasing on-target binding, minimizing off-target binding. We continue to progress working on assay stability of the new configuration chips that are stable over hundreds of cycles. All of these are challenges that require optimization, not innovation.

Speaker #4: As we look forward, what we're looking at are levers like increased further increasing on target binding, minimizing off-target binding, we continue to progress working on assay stability of the new configuration chips that are stable over hundreds of cycles, all of these are challenges that require optimization not innovation.

Ji-Yon Yi: Super helpful. Thank you so much, Parag.

Subbu Nambi: Super helpful. Thank you so much, Parag.

Speaker #3: Super helpful. Thank you so much, Parag.

Speaker #4: Yeah.

Parag Mallick: Yeah.

Speaker #2: Thank you. As a reminder to ask a question, you will need to press star 11 on your telephone and wait for your name to be announced.

Operator: Thank you. As a reminder, to ask a question, you will need to press star one one on your telephone and wait for your name to be announced. To withdraw your question, please press star one one again. Our next question comes from Dan Brennan from TD Cowen. Your line is now open.

Speaker #2: To withdraw your question, please press star 11 again. Our next question comes from Dan Brennan from TD Cowan. Your line is now open.

[Analyst] (TD Cowen): Hey, good morning. This is Kyle on for Dan. Thanks for taking the questions. You know, starting with this year, I know you said no material contribution from early access in terms of revenue and a modest contribution later this year from service, and reiterated the commercial launch for later this year. Do you anticipate any revenue at all from a commercial launch later this year? I think the street was modeling a few million dollars in revenue, you know, all the way out in Q4. Maybe building off of that, have you discussed anything new around, you know, pricing for the Voyager instrument? Thank you.

Kyle Boucher: Hey, good morning. This is Kyle on for Dan. Thanks for taking the questions. You know, starting with this year, I know you said no material contribution from early access in terms of revenue and a modest contribution later this year from service, and reiterated the commercial launch for later this year. Do you anticipate any revenue at all from a commercial launch later this year? I think the street was modeling a few million dollars in revenue, you know, all the way out in Q4. Maybe building off of that, have you discussed anything new around, you know, pricing for the Voyager instrument? Thank you.

Speaker #5: Hey, good morning. This is Kyle on for Dan. Thanks for taking the questions. So starting with this year, I know you said no material contribution from early access in terms of revenue and a modest contribution later this year from service and reiterated the commercial launch for later this year.

Speaker #5: But do you anticipate any revenue at all from a commercial launch later this year? I think the street was modeling a few million dollars in revenue all the way out in the fourth quarter.

Speaker #5: And then maybe building off of that, have you discussed anything new around pricing you.

Anna Mowry: Kyle, I can definitely give you a little bit more color there. As you reiterated, we don't see our early access engagements as a major driver of revenue that, although we do expect some modest services revenue later in the year, our revenue for 2026 will really come from two sources. First, I'm anticipating a portion of the Michael J. Fox grant funding to be recognized as revenue in 2026, with the remainder flowing into 2027. While what the work that we do for that grant may vary depending on the quarter, I think it's reasonable to expect some revenue coming in from that.

Speaker #3: Kyle, I can definitely give you a little bit more color there. As you reiterated, we don't see our early access engagements as a major driver of revenue.

Speaker #3: That although we do expect some modest services revenue later in the year, our revenue for 2026 will really come from two sources. First, I am anticipating a portion of the Michael J.

Speaker #3: Fox grant funding to be recognized as revenue in 2026 with the remainder flowing into 2027. While what the work that we do for that grant may vary depending on the quarter, I think it's reasonable to expect some revenue coming in from that.

Speaker #3: On top of that, with a handful of early access customers, converting to revenue within the year, I'm looking at a target of closer to, say, half a million dollars for 2026.

Anna Mowry: On top of that, with a handful of early access customers, converting to revenue within the year, I'm looking at a target of closer to, say, half a million dollars for 2026. The revenue ramp tied to instruments is really coming in 2027. On the pricing front, we don't have anything in addition, any changes from what we've talked about previously.

Speaker #3: The revenue ramp tied to instruments is really coming in 2027. On the pricing front, we don't have anything in any changes from what we've talked about previously.

Speaker #5: Got it. Thank you. And then maybe can you just give a little bit more color on how the early access program is going? Maybe some of the feedback you've received from these early customers? And then, I guess building on that, can you speak to how your sales funnel is building ahead of the commercial launch later this year?

[Analyst] (TD Cowen): Got it. Thank you. Maybe can you just give a little bit more color on how the early access program is going? You know, maybe some of the feedback you've received from these early customers. I guess building on that, can you speak to how your sales funnel is building, you know, ahead of the commercial launch later this year?

Kyle Boucher: Got it. Thank you. Maybe can you just give a little bit more color on how the early access program is going? You know, maybe some of the feedback you've received from these early customers. I guess building on that, can you speak to how your sales funnel is building, you know, ahead of the commercial launch later this year?

Speaker #4: Yeah, let me tackle—Kyle, let me tackle this. Sujal, I'll tackle the commercial pieces of that, and Parag can give you some of the early feedback, because really the early feedback is just from the Buck Institute and the Allen Institute, who've been working with us in the very early stages of the early access, or the late stages of their collaborations.

Parag Mallick: Yeah. Let me tackle, Kyle, let me tackle this issue. I'll tackle the commercial pieces of that, and Parag can give you some of the early feedback, because really, the early feedback is just from the Buck Institute and the Allen Institute, who've been working with us in the very early stages of the early access or the late stages of their collaborations. In terms of funnel, when we launched that early access program, one of the things that we said in our prepared remarks was that we elected to launch it earlier than previously communicated.

Sujal Patel: Yeah. Let me tackle, Kyle, let me tackle this issue. I'll tackle the commercial pieces of that, and Parag can give you some of the early feedback, because really, the early feedback is just from the Buck Institute and the Allen Institute, who've been working with us in the very early stages of the early access or the late stages of their collaborations. In terms of funnel, when we launched that early access program, one of the things that we said in our prepared remarks was that we elected to launch it earlier than previously communicated.

Speaker #4: In terms of the funnel, when we launched that early access program, one of the things that we said in our prepared remarks was that we elected to launch it earlier than previously communicated.

Speaker #4: And that is because the data quality and the excitement that we were seeing from customers based on the early data from the Buck and from the Allen Institute and our own internal data as well as through our partners who were who worked with us on the preprint that is out now, which is NSCI and Mount Sinai, all of that data was really exciting.

Parag Mallick: That is because the data quality and the excitement that we were seeing from customers based on the early data from the Buck and from the Allen Institute and our own internal data, as well as through our partners, who worked with us.

Sujal Patel: That is because the data quality and the excitement that we were seeing from customers based on the early data from the Buck and from the Allen Institute and our own internal data, as well as through our partners, who worked with us. on the preprint that is out now, which is NSCI and Mount Sinai. All of that data was really exciting. We elected to get out to watch. It's a little bit earlier than we were thinking. It's important to point out we have absolutely zero sales capacity in the company right now.

Sujal Patel: on the preprint that is out now, which is NSCI and Mount Sinai. All of that data was really exciting. We elected to get out to watch. It's a little bit earlier than we were thinking. It's important to point out we have absolutely zero sales capacity in the company right now. There's not a single salesperson in the company. The funnel build is something in earnest that we really just began. HUPO was a great opportunity to get in front of a lot of potential customers. In earnest, we will begin the sales capacity build this quarter and then continuing through the year with just a few targeted headcount. It's a pretty much a surgical strike sort of approach, right?

Speaker #4: We elected to get out to launch. Now, it's a little bit earlier than we were thinking it's important to point out we had absolutely zero sales capacity in the company right now.

Speaker #4: There's not a single salesperson in the company. And so the funnel build is something in earnest that we really just began. And so HUPO was a great opportunity to get in front of a lot of potential customers and in earnest, we will begin the sales capacity build this quarter and then continuing through the year with just a few targeted headcount and so it's a pretty pretty much a surgical strike sort of approach, right?

Sujal Patel: There's not a single salesperson in the company. The funnel build is something in earnest that we really just began. HUPO was a great opportunity to get in front of a lot of potential customers. In earnest, we will begin the sales capacity build this quarter and then continuing through the year with just a few targeted headcount. It's a pretty much a surgical strike sort of approach, right?

Speaker #4: It's not going to be a lot of commercial build, but we'll start to see that funnel build. Parag, do you want to talk about the feedback that we've received?

Sujal Patel: It's not gonna be a lot of commercial build, but we'll start to see that funnel build. Parag, do you wanna talk about the feedback that we've received?

Speaker #5: Yeah, absolutely. I think a highlight of the US HUPO meeting was very much Beer Get Chilling's presentation of her latest data, looking at both different brain regions of that complemented across these three XTG mouse models.

Parag Mallick: Yeah, absolutely. I think a highlight of the US HUPO meeting was very much Birgit Schilling's presentation of her latest data, looking at both different brain regions that complemented across these 3xTg mouse models, and then a study where she was looking at genetic alterations that predispose people, well, either predispose people to Alzheimer's disease or are protective. That has been a really big open question in the field about why there was this link between this gene called APOE and Alzheimer's disease, what actually occurred, how was this linked to tau? Her data, this proteoform level detail, really highlighted that those genotypes potentially led to changes in tau phosphorylation, and that was a critical predisposing factor.

Speaker #5: And then a study where she was looking at genetic alterations that predisposed people well, either predisposed people to Alzheimer's disease or are protective. And that had been a really big open question in the field about why there was this link between this gene called APOE and Alzheimer's disease, what actually occurred, how was this linked to Tau, and her data this proteoform level detail really highlighted that those genotypes potentially led to changes in Tau phosphorylation and that that was a critical predisposing factor.

Parag Mallick: That has been a really big open question in the field about why there was this link between this gene called APOE and Alzheimer's disease, what actually occurred, how was this linked to tau? Her data, this proteoform level detail, really highlighted that those genotypes potentially led to changes in tau phosphorylation, and that was a critical predisposing factor.

Speaker #5: Now, it's very early data, but it is exciting to have a tool that can allow us to finally see what the downstream consequences of this either protective or extremely deleterious mutation might be.

Parag Mallick: It's very early data, but it is exciting to have a tool that can allow us to finally see what the downstream consequences of this either protective or extremely deleterious mutation might be. I think we heard from, you know, other folks at the conference, both how excited they were to see the data, how much they appreciated the quality of the data, that the story itself and the multi-omic link was extremely exciting to them and something that they want the ability to be able to forge those connections and see things they haven't been able to see before. It was really exciting to get that feedback from the community.

Speaker #5: And so I think we heard from other folks at the conference both how excited they were to see the data, how much they appreciated the quality of the data, that the story itself and the multi-omic link was extremely exciting to them and something that they want the ability to be able to forge those connections and see things they haven't been able to see before.

Speaker #5: So it feedback from the community. Got it. Thank you.

Sujal Patel: Got it. Thank you.

Kyle Boucher: Got it. Thank you.

Operator: Thank you. I am showing no further questions at this time. Thank you for your participation in today's conference. This does conclude the program. You may now disconnect.

Q4 2025 Nautilus Biotechnology Inc Earnings Call

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