CJC-1295 + Ipamorelin (blend): Research overview, identity, and laboratory handling guide

Co-lyophilized GHRH analogue + selective GHS-R1a agonist research blend. Studied in vitro for GHRH-R / GHS-R co-stimulation work. Research use only. This guide covers identity, published research context, procurement checks, and storage — RUO only, no clinical claims.

What CJC-1295 + Ipamorelin (blend) is in published research

This blend co-lyophilizes a GHRH analogue (CJC-1295 No DAC / Modified GRF 1-29) with a selective GHS-R1a agonist (Ipamorelin) at equal mass. Published research has examined co-stimulation of GHRH-R and GHS-R as a reference paradigm for studying synergistic signaling at the somatotrope; this listing is structured so labs investigating that pathway can source both components as a single QC-traced unit.

Each lot ships with HPLC purity ≥99% reported separately for the GHRH analogue and the GHS peptide, and MS identity verification of each backbone. Net peptide content is reported per component on the CoA so molarity calculations remain accurate for split-channel assays.

Hold sealed vials at -20 °C protected from light. Reconstitute the entire blend in bacteriostatic water; aliquot into single-use volumes and freeze. Because two peptides share a vial, do not draw partial-component aliquots without confirming the as-reconstituted concentration on the CoA.

CoA covers per-component identity (MS), per-component purity (HPLC), as-blended mass ratio, and net peptide content per component. Batch records by lot are filed against the SKU.

The material class "GHRH + GHS blend (research)" helps procurement teams group CJC-1295 + Ipamorelin (blend) with related reference peptides during comparative studies.

Sequence and identity

CJC-1295 + Ipamorelin (blend) identity on the catalog: Components: CJC-1295 (No DAC) + Ipamorelin; Ratio (mg : mg): 1 : 1 by mass (CoA reports actual); Form: Co-lyophilized blend in a single vial; Component MW: 3,367.95 / 711.86 g/mol; Appearance: White lyophilized powder; Purity (HPLC) per component: ≥ 99%; Net peptide: Listed per component on CoA; Solubility: Soluble in bacteriostatic water. Copy these into receiving and LIMS before reconstitution.

Mechanisms studied in published research

Mechanism-focused research on CJC-1295 + Ipamorelin (blend) is typically conducted in cell lines or biochemical preparations that express the relevant receptor or binding protein for its class.

Design controls that include scrambled-sequence or orthogonal-receptor negative controls when your protocol evaluates CJC-1295 + Ipamorelin (blend) pharmacology in vitro.

Report effect sizes with lot number and CoA reference so results can be reproduced if the same CJC-1295 + Ipamorelin (blend) SKU is reordered later.

Avoid extrapolating in vitro binding or signaling readouts to whole-organism outcomes; RUO materials are not qualified for clinical investigation.

Procurement and identity verification

Request the lot-specific CoA for CJC-1295 + Ipamorelin (blend) at receipt. Verify SKU, variant size if applicable, and identity mass before the lot enters general storage.

Compare HPLC purity to your internal minimum for the peptide family. File chromatogram excerpts when your QMS requires raw data.

Enter net peptide content from the CoA into inventory before calculating molarity for CJC-1295 + Ipamorelin (blend) working stocks.

Attach purchase order, packing list, and CoA in one audit folder per lot.

Storage and reconstitution

Store lyophilized CJC-1295 + Ipamorelin (blend) sealed at -20 °C protected from light unless the CoA states otherwise.

Reconstitute with bacteriostatic water or a buffer validated for your assay pH. Aliquot to limit freeze-thaw.

For oxidation-sensitive sequences in CJC-1295 + Ipamorelin (blend), minimize open-vial time at room temperature during weighing.

See our lyophilized storage guide for institution-scale SOP examples and aliquot labeling conventions.

Comparative reference points

Researchers comparing CJC-1295 + Ipamorelin (blend) with adjacent catalog references often evaluate the following SKUs in parallel plates:

Use matched reconstitution buffers and stock concentrations when running comparative binding or signaling assays.

Document reviewers should cross-link this guide with the product certificate of analysis and internal receiving SOP.

When publishing methods, cite lot number, SKU, reconstitution buffer, and stock concentration so external labs can interpret your figures.

Institutional procurement may require RUO acknowledgment at checkout; store that acknowledgment beside batch records for audits.

If assay results drift across quarters, compare storage logs and CoA revision before questioning sequence integrity.

Third-party summaries, when available, should be filed as supplements—not replacements—for CoA identity data.

Document reviewers should cross-link this guide with the product certificate of analysis and internal receiving SOP.

When publishing methods, cite lot number, SKU, reconstitution buffer, and stock concentration so external labs can interpret your figures.

Institutional procurement may require RUO acknowledgment at checkout; store that acknowledgment beside batch records for audits.

If assay results drift across quarters, compare storage logs and CoA revision before questioning sequence integrity.

Third-party summaries, when available, should be filed as supplements—not replacements—for CoA identity data.

Document reviewers should cross-link this guide with the product certificate of analysis and internal receiving SOP.

When publishing methods, cite lot number, SKU, reconstitution buffer, and stock concentration so external labs can interpret your figures.

Institutional procurement may require RUO acknowledgment at checkout; store that acknowledgment beside batch records for audits.

If assay results drift across quarters, compare storage logs and CoA revision before questioning sequence integrity.

Third-party summaries, when available, should be filed as supplements—not replacements—for CoA identity data.

Document reviewers should cross-link this guide with the product certificate of analysis and internal receiving SOP.

When publishing methods, cite lot number, SKU, reconstitution buffer, and stock concentration so external labs can interpret your figures.

Institutional procurement may require RUO acknowledgment at checkout; store that acknowledgment beside batch records for audits.

If assay results drift across quarters, compare storage logs and CoA revision before questioning sequence integrity.

Third-party summaries, when available, should be filed as supplements—not replacements—for CoA identity data.

Document reviewers should cross-link this guide with the product certificate of analysis and internal receiving SOP.

When publishing methods, cite lot number, SKU, reconstitution buffer, and stock concentration so external labs can interpret your figures.

Institutional procurement may require RUO acknowledgment at checkout; store that acknowledgment beside batch records for audits.

If assay results drift across quarters, compare storage logs and CoA revision before questioning sequence integrity.

Third-party summaries, when available, should be filed as supplements—not replacements—for CoA identity data.

Document reviewers should cross-link this guide with the product certificate of analysis and internal receiving SOP.

When publishing methods, cite lot number, SKU, reconstitution buffer, and stock concentration so external labs can interpret your figures.

Institutional procurement may require RUO acknowledgment at checkout; store that acknowledgment beside batch records for audits.

If assay results drift across quarters, compare storage logs and CoA revision before questioning sequence integrity.

Third-party summaries, when available, should be filed as supplements—not replacements—for CoA identity data.

Document reviewers should cross-link this guide with the product certificate of analysis and internal receiving SOP.

When publishing methods, cite lot number, SKU, reconstitution buffer, and stock concentration so external labs can interpret your figures.

Institutional procurement may require RUO acknowledgment at checkout; store that acknowledgment beside batch records for audits.

If assay results drift across quarters, compare storage logs and CoA revision before questioning sequence integrity.

Third-party summaries, when available, should be filed as supplements—not replacements—for CoA identity data.

Document reviewers should cross-link this guide with the product certificate of analysis and internal receiving SOP.

When publishing methods, cite lot number, SKU, reconstitution buffer, and stock concentration so external labs can interpret your figures.

Institutional procurement may require RUO acknowledgment at checkout; store that acknowledgment beside batch records for audits.

If assay results drift across quarters, compare storage logs and CoA revision before questioning sequence integrity.

Third-party summaries, when available, should be filed as supplements—not replacements—for CoA identity data.