Climb Bio Announces Initial Phase 1b Data Demonstrating On-Target Clinical Activity for Budoprutug in Immune Thrombocytopenia at EHA Congress 2026

Rhea-AI Summary

Climb Bio (Nasdaq: CLYM) reported initial Phase 1b data for budoprutug, an anti-CD19 antibody, in adults with primary immune thrombocytopenia at EHA 2026.

Among 15 heavily pretreated patients, budoprutug showed an encouraging safety profile, >90% B-cell depletion, and higher platelet counts, supporting continued evaluation.

AI-generated analysis. Not financial advice.

Positive

• No serious adverse events, discontinuations, or infusion reactions at 250 mg and 500 mg
• All reported adverse events were Grade 1 or Grade 2
• B-cell levels in 250 mg cohort depleted by >90% by Week 4
• Mean platelet count in 250 mg cohort increased by 111,000/µL at Week 24
• Durable platelet responses in 4 of 6 patients in 250 mg cohort
• Three of four rituximab-exposed patients responded to budoprutug

Negative

• Only 15 patients enrolled across 250 mg and 500 mg cohorts as of June 1, 2026
• Median follow-up limited to 12 weeks in 500 mg cohort
• Enrollment in 1000 mg cohort ongoing, so high-dose safety and efficacy not yet reported

Key Figures

Patients enrolled: 15 patients Dose cohorts: 250 mg, 500 mg, 1000 mg Median follow-up: 38 and 12 weeks +5 more

8 metrics

Patients enrolled 15 patients Phase 1b budoprutug ITP trial, 250 mg and 500 mg cohorts as of June 1, 2026

Dose cohorts 250 mg, 500 mg, 1000 mg Three ascending intravenous budoprutug doses in Phase 1b/2a ITP study

Median follow-up 38 and 12 weeks Follow-up for 250 mg and 500 mg ITP cohorts respectively

Prior therapy lines 6 to 7.5 lines Median prior lines of therapy in heavily pretreated ITP patients

B-cell depletion Over 90% Average B-cell level reduction by Week 4 in 250 mg cohort

Platelet increase 111,000 platelets/µL Mean platelet count change at Week 24 in 250 mg cohort

Durable responders 4 of 6 patients Durable platelet responses in 250 mg cohort

Rituximab-pretreated response 3 of 4 patients Patients previously treated with rituximab responding to budoprutug

Market Reality Check

Price: $10.80 Vol: Volume 575,290 is below t...

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$10.80 Last Close

Volume Volume 575,290 is below the 20-day average of 1,075,607, suggesting a relatively muted pre-news session. low

Technical Shares at $10.80 are trading above the 200-day MA of $5.24 and about 13.5% below the 52-week high of $12.48.

Peers on Argus

CLYM was down 3.01% while several biotech peers like CABA (-3.49%) and KYTX (-0....

1 Down

CLYM was down 3.01% while several biotech peers like CABA (-3.49%) and KYTX (-0.78%) were also negative, but only one peer appeared in the momentum scanner and sector-wide coordination was limited.

Historical Context

5 past events · Latest: Jun 05 (Positive)

Pattern 5 events

Date	Event	Sentiment	Move	Catalyst
Jun 05	Clinical data update	Positive	-3.3%	Initial Phase 1 safety and modeling data for CLYM116 in IgA nephropathy.
May 26	Conference preview	Positive	+3.5%	Announcement of ERA 2026 presentations for CLYM116 and budoprutug.
May 14	Clinical data preview	Positive	-0.7%	Planned EHA 2026 poster with early budoprutug ITP data at 24 weeks.
May 12	Investor conferences	Neutral	+0.5%	Participation in H.C. Wainwright and Jefferies investor conferences.
May 07	Earnings and updates	Neutral	-2.5%	Q1 2026 results, pipeline milestones, and $110M private placement details.

Pattern Detected

Recent clinically focused and corporate updates have often been followed by mixed to negative price reactions, even when the news itself is constructive.

Recent Company History

Over the last month, Climb Bio has reported multiple R&D and corporate milestones. Clinical updates for CLYM116 and budoprutug, conference presentations, and Q1 2026 results with a completed $110 million private placement have highlighted active development across renal and autoimmune indications. Price reactions have been split, with some clinical and conference news met by declines (e.g., -3.3%, -2.54%) and others modest gains. Today’s ITP Phase 1b data further extends this pattern of steady pipeline disclosure with uneven market response.

Regulatory & Risk Context

Active S-3 Shelf

Shelf Active

Active S-3 Shelf Registration 2026-05-29

An effective S-3 shelf dated May 29, 2026 registers up to 11,587,000 shares for resale by selling stockholders, consisting of 9,481,000 outstanding shares and 2,106,000 shares issuable on prefunded warrant exercise. The company states it will not receive proceeds from these resales, aside from potential cash from warrant exercises.

Market Pulse Summary

This announcement highlights initial Phase 1b data for budoprutug in primary ITP, with over 90% B-ce...

Analysis

This announcement highlights initial Phase 1b data for budoprutug in primary ITP, with over 90% B-cell depletion and a mean platelet increase of 111,000/µL in heavily pretreated patients, alongside a favorable safety profile. Prior months featured multiple data and corporate updates with varied market reactions. Investors may watch for additional high-dose cohort readouts by year-end 2026 and any further use of the effective shelf covering 11,587,000 resale shares.

Key Terms

phase 1b/2a, immune thrombocytopenia, monoclonal antibody, b-cell depletion, +4 more

8 terms

phase 1b/2a medical

"The ongoing Phase 1b/2a study is evaluating budoprutug in patients..."

Phase 1b/2a is a combined early-stage clinical study that first tests safety and optimal dosing in a small group and then expands to look for initial signs that the drug works in the target patients. Think of it as a prototype test followed by a small pilot run: it helps companies decide whether to invest in larger, more expensive trials. Investors watch these results because they reduce scientific uncertainty and can sharply affect a drug’s value and development timeline.

immune thrombocytopenia medical

"in adults with primary immune thrombocytopenia (ITP) demonstrating an encouraging..."

Immune thrombocytopenia is a blood disorder in which the body's immune system mistakenly destroys platelets, the small cells that help blood clot, causing easy bruising, bleeding and a low platelet count. Investors care because the condition drives demand for diagnostic tests, treatments and clinical trials, affects regulatory and reimbursement decisions, and can influence revenue and risk profiles for companies developing therapies—think of it as the immune system removing the repair crew needed to stop leaks.

monoclonal antibody medical

"budoprutug, an anti-CD19 monoclonal antibody, in adults with primary..."

A monoclonal antibody is a laboratory-made protein designed to recognize and attach to a specific target in the body, such as a disease-causing substance or cell. It functions like a highly precise lock-and-key tool, helping to treat or detect illnesses. For investors, companies developing monoclonal antibodies can represent promising opportunities in the healthcare sector, especially as these treatments often address unmet medical needs.

b-cell depletion medical

"robust B-cell depletion, and meaningful platelet responses in heavily pretreated..."

B-cell depletion is a medical treatment strategy that lowers or removes B cells, a type of white blood cell that makes antibodies and helps coordinate immune responses. For investors, it matters because therapies that deplete B cells can be major products for autoimmune diseases, certain blood cancers, or organ transplant care, affecting sales potential, safety profiles, and regulatory risk; think of it like reducing a specific unit in an army to stop friendly fire but increasing vulnerability to other attacks.

serious adverse events medical

"with no serious adverse events, no treatment discontinuations due to adverse..."

Serious adverse events are significant problems or negative outcomes that occur during a medical treatment or clinical trial, such as severe side effects, hospitalizations, or life-threatening conditions. They matter to investors because such events can impact a company's reputation, lead to regulatory scrutiny, or delay the development of new products, ultimately affecting the company’s financial performance.

grade 1 to grade 2 medical

"and no infusion related reactions; all adverse events were Grade 1 to Grade 2"

A "grade 1 to grade 2" description denotes a change from a mild to a moderate level of a symptom, side effect or clinical finding on a standard medical severity scale used in trials and regulatory reports. For investors, it signals that an issue moved from minor and easily managed to more noticeable and potentially requiring treatment or monitoring; like a small crack becoming a hairline fracture that may need closer attention, it can affect product risk profiles and market perception.

rituximab medical

"Of the four patients who had previously been treated with rituximab, three..."

Rituximab is a lab-made antibody drug that seeks out and removes a specific kind of white blood cell involved in certain blood cancers and autoimmune diseases, like a guided missile that finds its target. It matters to investors because regulatory approvals, clinical trial results, patent status and the arrival of lower-cost copies can sharply change sales, company value and future cash flow for firms that make or sell the therapy.

prefunded warrants financial

"2,106,000 shares issuable upon exercise of prefunded warrants held by one..."

Prefunded warrants are a security that gives the holder the right to convert the warrant into a share after paying a very small remaining amount because almost the full purchase price was paid upfront. They matter to investors because exercising them increases the company’s outstanding shares (dilution) and can provide immediate cash to the issuer while allowing holders to bypass ownership limits or simplify timing, similar to buying a nearly-complete gift card that only needs a tiny top-up to use.

AI-generated analysis. Not financial advice.

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Data demonstrate favorable safety and tolerability profile, robust B-cell depletion, and encouraging platelet responses in heavily pretreated patients with primary immune thrombocytopenia

Enrollment ongoing in the high dose cohort, with additional data anticipated by year-end 2026

WELLESLEY HILLS, Mass., June 11, 2026 (GLOBE NEWSWIRE) -- Climb Bio, Inc. (Nasdaq: CLYM), a clinical stage biotechnology company developing therapeutics for patients with immune-mediated diseases, today announced initial data from the ongoing Phase 1b portion of its Phase 1b/2a study evaluating budoprutug, an anti-CD19 monoclonal antibody, in adults with primary immune thrombocytopenia (ITP) demonstrating an encouraging safety and tolerability profile, robust B-cell depletion, and meaningful platelet responses in heavily pretreated patients. The initial data are being presented at the European Hematology Association (EHA) Congress 2026, which is being held on June 11-14, 2026, in Stockholm, Sweden.

The ongoing Phase 1b/2a study is evaluating budoprutug in patients with primary ITP to inform dose and regimen selection and assess safety and the depth and duration of platelet response and B-cell depletion. Initial safety and efficacy data are available from the 250 mg cohort, and initial safety data are available from the 500 mg cohort. Enrollment in the 1000 mg cohort is ongoing.

“Patients with chronic ITP often cycle through multiple therapies without achieving a sustained response,” said Edgar D. Charles, M.D., Chief Medical Officer of Climb Bio. “These initial data suggest that targeting CD19 with budoprutug may offer a differentiated approach in ITP, enabling robust B-cell depletion, durable platelet responses, and an acceptable safety and tolerability profile. Importantly, we observed platelet responses in several patients who had been previously treated with rituximab, highlighting the potential to address a high unmet need population where available treatment options remain limited. Taken together, these data demonstrate biological activity of budoprutug in ITP, and importantly, provide proof-of-concept in a non-renal autoimmune indication. We look forward to sharing additional data from this study later in the year.”

Study Design and Data Highlights

• The Phase 1b portion of the Phase 1b/2a study (NCT07043946) is evaluating three ascending doses (250 mg, 500 mg and 1000 mg) of intravenous budoprutug, administered in two doses 14 days apart, in adults with primary ITP who have received at least one prior therapy
• As of June 1, 2026, 15 patients had been enrolled across the 250 mg (n=6) and 500 mg (n=9) dose cohorts, median follow-up was 38 weeks and 12 weeks for the 250 mg and 500 mg cohorts respectively.
• Patients enrolled were heavily pretreated, with a median of 6 to 7.5 prior lines of therapy and disease duration ranging from 0.5 to 40 years
• Budoprutug was generally well tolerated at both the 250 mg and 500 mg dose levels, with no serious adverse events, no treatment discontinuations due to adverse events, and no infusion related reactions; all adverse events were Grade 1 to Grade 2
• In the 250 mg dose cohort, B-cell levels were depleted by an average of over 90% by Week 4 and mean platelet count increased by 111,000 platelets/µL at Week 24
• Durable platelet responses were achieved in four out of six patients in the 250 mg dose cohort, with two out of six patients experiencing platelet levels >100 x 10³/µL for over 24 weeks
  • Of the four patients who had previously been treated with rituximab, three responded to treatment with budoprutug, two with durable and complete responses
• Results to date support continued clinical evaluation of budoprutug in ITP; enrollment in the 1000 mg cohort is ongoing

The poster presentation is available on the Pipeline & Science—Publications page of the Company’s website here.

About Climb Bio, Inc.
Climb Bio, Inc. is a clinical-stage biotechnology company with a mission to deliver high impact, disease-modifying medicines for individuals living with immune-mediated diseases, including those affecting kidney health. The Company’s pipeline includes, budoprutug, an anti-CD19 monoclonal antibody that has potential to treat a broad range of B-cell mediated diseases, and CLYM116, an anti-APRIL monoclonal antibody being developed for IgA nephropathy. For more information, please visit climbbio.com. 

About Budoprutug
Budoprutug is a clinical-stage, anti-CD19 monoclonal antibody with the potential to address a broad range of B-cell mediated, immune-driven diseases. Designed with enhanced effector function and low picomolar affinity, budoprutug targets and depletes CD19-expressing B cells, including plasmablasts and certain plasma cells, key sources of pathogenic autoantibodies. Early clinical data suggest budoprutug may offer durable B-cell depletion, rapid reductions in autoantibodies, and clinical remission in primary membranous nephropathy (pMN). Budoprutug is being evaluated in clinical trials for pMN, immune thrombocytopenia (ITP), and systemic lupus erythematosus (SLE). A subcutaneous formulation is also in development to enable broader patient access. Budoprutug has been granted Orphan Drug Designation and Fast Track Designation by the FDA for the treatment of pMN.

About Immune Thrombocytopenia
Immune thrombocytopenia (“ITP”) is a rare autoimmune disorder characterized by low platelet counts and an increased risk of bleeding, which can include serious mucosal, gastrointestinal and intracranial bleeding events. There are approximately 85,000 ITP patients in the United States alone. Approximately 40% to 50% of patients require chronic therapy over time, and approximately 20% fail multiple lines of therapy, underscoring the need for novel disease-modifying approaches with the potential to deliver durable responses while maintaining a favorable safety and tolerability profile.

Forward-Looking Statements
This press release contains “forward-looking statements” within the meaning of the Private Securities Litigation Reform Act of 1995, including without limitation statements regarding: future expectations, plans and prospects for Climb Bio; expectations regarding the therapeutic benefits, clinical potential and clinical development of budoprutug; the anticipated timelines for announcing data from Climb Bio’s ongoing and planned clinical trials; the anticipated timelines for enrolling patients in Climb Bio’s ongoing and planned clinical trials; plans for the development strategy for budoprutug; potential commercial opportunity for budoprutug in immune thrombocytopenia; and other statements containing the words “anticipate,” “believe,” “continue,” “could,” “estimate,” “expect,” “intend,” “may,” “plan,” “potential,” “predict,” “project,” “should,” “suggest,” “target,” “would,” “will,” “working” and similar expressions. Forward-looking statements are based on management’s current expectations of future events and are subject to a number of risks and uncertainties that could cause actual results to differ materially and adversely from those set forth in, or implied by, such forward-looking statements. Climb Bio may not actually achieve the plans, intentions or expectations disclosed in these forward-looking statements, and you should not place undue reliance on these forward-looking statements. These risks and uncertainties include, but are not limited to, important risks and uncertainties associated with: the ability of Climb Bio to timely and successfully achieve or recognize the anticipated benefits of its acquisition of Tenet Medicines, Inc. and its technology transfer and exclusive license agreement with Beijing Mabworks Biotech Co., Ltd.; Climb Bio’s ability to advance budoprutug and CLYM116 on the timelines expected or at all and to obtain and maintain necessary approvals from the U.S. Food and Drug Administration and other regulatory authorities; obtaining and maintaining the necessary approvals from investigational review boards at clinical trial sites and independent data safety monitoring boards; replicating in clinical trials positive results found in early-stage clinical trials or nonclinical studies; competing successfully with other companies that are seeking to develop treatments for primary membranous nephropathy, immune thrombocytopenia, systemic lupus erythematosus, IgA nephropathy and other immune-mediated diseases; maintaining or protecting intellectual property rights related to budoprutug, CLYM116 and/or its other product candidates; managing expenses; changes in applicable laws or regulation; the possibility that Climb Bio may be adversely affected by other economic, business and/or competitive factors; and raising the substantial additional capital needed, on the timeline necessary, to continue development of budoprutug, CLYM116 and any other product candidates Climb Bio may develop. For a discussion of other risks and uncertainties, and other important factors, any of which could cause Climb Bio’s actual results to differ materially from those contained in the forward-looking statements, see the “Risk Factors” section, as well as discussions of potential risks, uncertainties and other important factors, in Climb Bio’s most recent filings with the U.S. Securities and Exchange Commission. In addition, the forward-looking statements included in this press release represent Climb Bio’s views as of the date hereof and should not be relied upon as representing Climb Bio’s views as of any date subsequent to the date hereof. Climb Bio anticipates that subsequent events and developments will cause Climb Bio’s views to change. However, while Climb Bio may elect to update these forward-looking statements at some point in the future, Climb Bio specifically disclaims any obligation to do so, except as required by law.

Investors and Media
Carlo Tanzi, Ph.D.
Kendall Investor Relations
ctanzi@kendallir.com

FAQ

What Phase 1b results did Climb Bio (CLYM) report for budoprutug in ITP at EHA 2026?

Climb Bio reported initial Phase 1b data showing on-target clinical activity of budoprutug in primary ITP. According to Climb Bio, results included robust B-cell depletion, higher platelet counts, and an encouraging safety profile in heavily pretreated adults.

How many patients were included in Climb Bio’s Phase 1b budoprutug ITP data for CLYM?

According to Climb Bio, 15 adults with primary immune thrombocytopenia were enrolled across the 250 mg (n=6) and 500 mg (n=9) cohorts. Median follow-up was 38 weeks in the 250 mg group and 12 weeks in the 500 mg group.

What safety profile did budoprutug show in Climb Bio’s Phase 1b ITP study (CLYM)?

Budoprutug was generally well tolerated at 250 mg and 500 mg in the Phase 1b ITP study. According to Climb Bio, there were no serious adverse events, no treatment discontinuations, no infusion-related reactions, and all adverse events were Grade 1 or Grade 2.

What platelet response data did Climb Bio report for budoprutug in ITP patients (CLYM)?

In the 250 mg cohort, mean platelet count increased by 111,000 platelets/µL at Week 24. According to Climb Bio, four of six patients achieved durable platelet responses, and two maintained platelet levels above 100×10³/µL for more than 24 weeks.

How did prior rituximab-treated ITP patients respond to budoprutug in Climb Bio’s CLYM trial?

Among four patients previously treated with rituximab, three responded to budoprutug. According to Climb Bio, two of these patients achieved durable and complete platelet responses, suggesting activity in a heavily pretreated, high unmet-need subgroup.

What are the next steps for Climb Bio’s budoprutug ITP program (NASDAQ: CLYM)?

Enrollment is ongoing in the 1000 mg cohort of the Phase 1b/2a study. According to Climb Bio, results to date support continued clinical evaluation in primary ITP, with additional data from the trial anticipated by year-end 2026.