Aplisol

Tuberculin Purified Protein Derivative (PPD) is a sterile, non-infectious diagnostic antigen used in the Mantoux skin test to detect latent tuberculosis infection by identifying delayed-type hypersensitivity reactions in the skin.

The standard adult dosage for the Tuberculin Purified Protein Derivative (PPD) skin test is a single intradermal injection of 0.1 mL of the 5 TU (Tuberculin Units) strength. This dose is consistent across all adult populations, regardless of weight or age, as it is designed to provide a standardized amount of antigen to trigger a measurable immune response.

In some specific clinical protocols, such as 'two-step testing' for healthcare workers, a second 0.1 mL dose may be administered 1 to 3 weeks after the initial test if the first test was negative. This is done to 'boost' the immune memory in individuals whose sensitivity to the antigen may have waned over many years, ensuring a more accurate baseline for future testing.

The pediatric dosage for Tuberculin PPD is identical to the adult dosage: 0.1 mL of the 5 TU strength administered intradermally. The American Academy of Pediatrics (AAP) and the Centers for Disease Control and Prevention (CDC) recommend this standardized dose for infants, children, and adolescents. There is no evidence that the dose needs to be adjusted for body surface area or age in the pediatric population, as the skin's immunological capacity to respond to the antigen is sufficiently developed even in early infancy.

Renal Impairment

No dosage adjustments are required for patients with renal (kidney) impairment. Since the PPD test is a localized diagnostic procedure with minimal systemic absorption, the kidneys are not responsible for clearing the drug in a way that would require dose modification.

Hepatic Impairment

No dosage adjustments are necessary for patients with hepatic (liver) impairment. The metabolism of the PPD proteins occurs locally in the skin and through the lymphatic system, rather than through the cytochrome P450 system in the liver.

Elderly Patients

While the dose remains 0.1 mL, healthcare providers must be aware that elderly patients may exhibit 'anergy' (a lack of immune response) due to a naturally weakened immune system (immunosenescence). This can lead to false-negative results. In these cases, a two-step testing procedure is often recommended to accurately identify latent infection.

Tuberculin PPD must be administered using the Mantoux technique by a trained healthcare professional. It is not for self-administration. The procedure involves:

1. 1Site Selection: Usually the volar surface (inner side) of the forearm, about 2 to 4 inches below the elbow.
2. 2Injection: Using a tuberculin syringe with a short (1/4 to 1/2 inch) 26- or 27-gauge needle, the provider inserts the needle bevel-up at a 5- to 15-degree angle into the superficial layers of the skin.
3. 3The Wheal: A successful injection will produce a pale, raised bump (wheal) approximately 6 to 10 mm in diameter. If no wheal appears, the injection was too deep, and the test must be repeated on the other arm or at least 2 inches away from the original site.
4. 4Storage: Vials must be stored in a refrigerator at 2°C to 8°C (36°F to 46°F) and protected from light. Once a vial is opened, it must be discarded after 30 days.

Because the Tuberculin PPD test is a diagnostic procedure rather than a daily medication, a 'missed dose' refers to a missed appointment for reading the test. The test must be read by a healthcare professional 48 to 72 hours after the injection. If you miss this window, the results are considered invalid. You will likely need to wait at least one week before the test can be repeated to avoid interference from the previous injection.

Systemic overdose of Tuberculin PPD is extremely rare because it is administered in such small, controlled volumes (0.1 mL). However, an accidental subcutaneous (deeper) injection or an excessive dose could lead to a severe local reaction, including extensive swelling, pain, or even tissue necrosis (skin death) at the injection site. There is no specific 'antidote' for PPD; treatment focuses on managing the local inflammation and monitoring for rare systemic allergic reactions.

> Important: Follow your healthcare provider's dosing instructions. Do not adjust your dose or attempt to interpret the skin reaction yourself without medical guidance.

The most common side effects of Tuberculin Purified Protein Derivative (PPD) are localized to the site of the injection. These are typically mild and represent the body's natural response to the antigen.

• Pain or Tenderness: A stinging or burning sensation during the injection is common. Some soreness at the site may persist for 24 to 48 hours.
• Pruritus (Itching): The injection site may become itchy as the immune response develops. Patients are advised not to scratch, as this can cause irritation or secondary infection.
• Erythema (Redness): Redness around the injection site is very common. It is important to note that redness alone is NOT used to determine a positive result; only the hardness (induration) is measured.
• Edema (Swelling): A slight puffiness at the site is expected as the immune system recruits fluid and cells to the area.

Tuberculin Purified Protein Derivative (PPD) is a diagnostic tool and must be handled with care. It is vital to understand that a positive PPD test does not necessarily mean you have active, contagious tuberculosis; it means you have been infected with the bacteria at some point. Conversely, a negative test does not 100% rule out TB, especially in those with severely weakened immune systems. The timing of the reading (48-72 hours) is critical; reading the test too early or too late will result in an inaccurate diagnosis, potentially leading to unnecessary treatment or a missed infection.

No FDA black box warnings for Tuberculin Purified Protein Derivative. It has a long history of safe use in public health screening programs worldwide.

• Allergic Reactions / Anaphylaxis Risk: Although rare, systemic allergic reactions can occur. Facilities administering the test must have epinephrine and other emergency supplies available to treat anaphylaxis. Patients with a known history of severe reactions to previous tuberculin tests should not receive the PPD skin test.

There are no drugs that are strictly contraindicated in the sense of causing a lethal chemical reaction with PPD. However, certain combinations are avoided because they make the test result completely uninterpretable.

• Live Virus Vaccines (e.g., MMR, Varicella, Yellow Fever): Live vaccines can temporarily suppress the body's cellular immune response. If a live vaccine is given shortly before a PPD test, it can cause a false-negative result. The PPD test should be administered either on the same day as the live vaccine or at least 4 to 6 weeks afterward.

These interactions may not prevent the test from being performed, but they require careful consideration when interpreting the results.

• Systemic Corticosteroids (e.g., Prednisone): High doses of steroids (equivalent to 15mg/day of prednisone or more for 2 weeks) suppress the T-cell response required for a positive PPD test. This can lead to false negatives.

There are specific circumstances where Tuberculin Purified Protein Derivative (PPD) must NEVER be used because the risk of a severe reaction outweighs any diagnostic benefit.

• Previous Severe Reaction: If a patient has a documented history of a severe reaction to PPD, such as vesiculation (blistering), ulceration, or necrosis (tissue death) at the injection site, the test is absolutely contraindicated. Re-exposure can cause an even more intense, painful, and scarring local reaction.
• Known Hypersensitivity to Components: Patients with a known allergy to any component of the formulation, including stabilizers like Polysorbate 80 or preservatives like Phenol, should not receive the injection. Anaphylaxis could occur.
• Documented Positive TB Test: If a person has already had a clearly documented positive PPD test or a positive TB blood test (IGRA) in the past, there is no clinical reason to repeat the skin test. It will likely remain positive, and the risk of a severe local reaction increases with repeated testing.

Tuberculin Purified Protein Derivative is considered safe for use during pregnancy. According to the CDC and the American College of Obstetricians and Gynecologists (ACOG), pregnancy does not diminish the skin's sensitivity to PPD, nor does the test pose a risk to the developing fetus. There is no evidence of teratogenicity (birth defects) because the PPD proteins do not enter the systemic circulation in significant amounts. Screening pregnant women for TB is particularly important because active TB during pregnancy can lead to poor maternal and neonatal outcomes, including low birth weight and congenital TB.

It is safe to receive a PPD skin test while breastfeeding. The PPD proteins are not absorbed into the bloodstream in quantities that would allow them to pass into breast milk. There is no risk to the nursing infant, and breastfeeding does not need to be interrupted. The diagnostic benefits of identifying and treating TB in a breastfeeding mother are critical for protecting the infant from exposure to active disease.

Tuberculin PPD is approved and widely used in the pediatric population, including infants. It is the standard method for TB screening in children. Healthcare providers must be careful to ensure the injection is truly intradermal, as children have thinner skin. In very young infants (under 6 months), the immune system may be slightly less responsive, but the 5 TU dose remains the standard. The test is NOT used to diagnose TB in children who have recently received certain live vaccines until the appropriate waiting period has passed.

Tuberculin Purified Protein Derivative (PPD) functions as a diagnostic provocateur of the cell-mediated immune system. The molecular mechanism involves the recognition of mycobacterial antigens by sensitized T-lymphocytes. Specifically, the PPD contains proteins like ESAT-6 and CFP-10 (though in a crude mixture compared to modern blood tests). When these proteins are introduced into the dermis, they are taken up by Antigen-Presenting Cells (APCs), such as dendritic cells. These APCs present the PPD fragments on their surface via Major Histocompatibility Complex (MHC) class II molecules. Sensitized CD4+ T-helper cells (Th1 cells) recognize these complexes and secrete pro-inflammatory cytokines, primarily Interferon-gamma (IFN-γ) and Tumor Necrosis Factor-alpha (TNF-α). This triggers a cascade that results in the characteristic firm swelling (induration) at the site.

The pharmacodynamics of PPD are characterized by the 'time-to-reaction.' The onset of the visible immune response typically begins 5 to 6 hours after injection, peaks between 48 and 72 hours, and slowly subsides over several days or weeks. The relationship between the dose (5 TU) and the response (diameter of induration) is standardized; however, the magnitude of the response is governed by the host's 'immunological memory' rather than the drug's concentration alone. Tolerance does not develop in the traditional sense, but repeated frequent testing can lead to a 'booster effect.'