AAV-tMCK-mCherry (AAV Serotype 1)

SKU:BHV21500245
Overview
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Recombinant AAV (AAV2/1) expressing tMCK-mCherry under tMCK for Skeletal muscle research.
Promoter tMCK
Transgene tMCK-mCherry
Reporter/Tag mCherry
Function Control/Fluorescent Proteins
Cell Type Skeletal muscle
Available Options

Select the AAV variant that best fits your experiment. Availability and lead time may vary by option.

  • Options:
    • Serotype: AAV2/1
    • Titer: 1x1013 VG/mL
    • Size (2) — 30 uL (Std Pack), 10 uL (Trial Pack)
  • Lead time: pre-made stock typically ships within 1–2 business days; other serotypes available to order with a 2-week lead time.
  • Storage: -80°C
  • Shipping: cold-chain shipment (typically with ice packs).
  • Upon receipt: store at the recommended temperature as soon as possible; avoid repeated freeze–thaw cycles.
  • Sales terms and conditions: Please review prior to ordering.
Options selector
Catalog no. Serotype Titer Size
SL101516-30UL AAV2/1
Field Specification
Cellular Localization Cytosolic
Form Frozen liquid
Function
  • Control/Fluorescent Proteins
Plasmid Backbone pAAV (AAV2 ITR)
Product Type
  • Vectors & Viruses, Adeno-associated viruses (AAVs)
Promoter tMCK
Reporter mCherry
Serotype AAV2/1
Storage -80°C
AAV2/1 Vector

AAV-tMCK-mCherry

tMCK Promoter • pAAV (AAV2 ITR) • Broad CNS and muscle tropism

BHV21500245

Research Background

Fluorescent reporter and control vectors are foundational tools for validating delivery, benchmarking expression levels, and serving as inert controls in experimental designs. AAV2/1 has broad CNS and muscle tropism.

The tMCK (truncated muscle creatine kinase) promoter restricts expression to striated muscle, supporting skeletal and cardiac muscle targeting. The plasmid backbone is pAAV (AAV2 ITR).

What This AAV Enables

Transgene Function

tMCK-mCherry is the encoded payload for this construct. A mCherry reporter tag is co-expressed to facilitate detection and validation of transduction.

Expression Pattern

Expression is constitutive—the transgene is continuously driven by the promoter without requiring an external trigger. The promoter is designed for expression restricted to skeletal muscle fibers.

Capsid Tropism

AAV2/1 has broad CNS and muscle tropism and is widely used for both in vivo and ex vivo applications.

Common Applications

  • In vivo gene delivery
  • Cell labeling
  • Promoter testing
  • Transduction benchmarking

Experimental Considerations

  • Allow sufficient expression time for AAV2/1 in your target tissue (often 2–4 weeks in vivo).
  • Verify targeting and expression level in a pilot cohort before committing to large study groups.
  • Use appropriate controls: tMCK-mCherry-negative or null-vector matched for serotype and dose.
  • Confirm expression distribution with immunostaining, in situ hybridization, or imaging as appropriate.

Controls and Best Practices

Recommended controls include: (1) a null or fluorophore-only matched vector to separate delivery effects from payload effects; (2) tissue-matched positive controls to confirm transduction efficiency at your injection coordinates and timepoint; (3) dose-response characterization if the phenotype is sensitive to expression level; and (4) replication across biological cohorts or preparations to confirm robustness.

High-quality recombinant adeno-associated virus vectors for gene delivery research, produced using a modified helper-free production system.

Production System

All pre-packaged recombinant adeno-associated viruses (rAAVs) are produced using a modified helper-free production system, optimized for high-yield and safe viral vector generation. The rAAV cis plasmids contain the left and right inverted terminal repeats (ITRs) derived from wild-type AAV serotype 2, which are essential for genome replication, packaging, and integration into host cells. The final rAAV serotype is determined by the capsid protein provided during vector packaging, enabling precise control over tissue tropism and transduction efficiency for a wide range of experimental applications.

Purification & Quality Control

All pre-made rAAV vectors undergo rigorous purification procedures to achieve in vivo-grade standards. This process removes cellular debris, proteins, and other contaminants, producing highly pure viral preparations suitable for both in vitro tissue culture experiments and direct administration in animal studies. In addition, each vector batch is subjected to comprehensive quality control, including assessment of viral genome integrity, particle concentration, and functional transduction efficiency, ensuring consistent performance and reliability.

Applications

By combining high-quality vector design, stringent purification, and extensive quality control, these pre-packaged rAAVs provide researchers with a ready-to-use, safe, and efficient solution for gene delivery. They are ideal for studies ranging from basic research to preclinical applications, including gene function analysis, disease modeling, and therapeutic development.

Helper-Free System In Vivo Grade Serotype 2 ITRs QC Validated Ready-to-Use

High-quality recombinant adeno-associated virus vectors

Inverted Terminal Repeats (ITRs)

Left ITR Derived from wild-type AAV serotype 2; fully sequence-verified
Right ITR Derived from wild-type AAV serotype 2; fully sequence-verified

Transgene Cassette (ITR to ITR)

Fully sequence-verified via WPS of the NanoPore platform

Purification & Quantification

Purity In vivo-grade; super-purified by two rounds of CsCl density-gradient ultracentrifugation
Titration Determined via qPCR using ITR-specific primers and probe; reported as viral genome copies per milliliter (VG/mL)

Quality Control & Availability

Endotoxin Assay Endotoxin level as measured by the Limulus amebocyte lysate (LAL) assay to ensure in vivo grade of AAV vector
In Stock Yes, immediately available and ships the same day upon order confirmation

Can’t find the AAV you need—or require a custom design and packaging service? We offer end-to-end support for diverse research and therapeutic needs, including vector design and cloning, AAV packaging services (serotype/capsid selection and production), QC & characterization (project-appropriate testing and documentation), and library preparation for pooled or library-style workflows (project dependent). Click Talk to a Scientist to submit a request form, email us at support@biohippo.com, or explore our Research Services for additional support. Our team will be in contact with you shortly.

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