SC to look into feasibility of NAT for blood transfusion

SC to Look into Feasibility of NAT for Blood Transfusion — UPSC Study Note

1. At a Glance

The Supreme Court of India is examining whether blood banks should be mandatorily required to conduct Nucleic Acid Test (NAT) for screening blood donations before transfusion. [S1]
NAT is a highly sensitive molecular technique that detects genetic material (DNA/RNA) of viruses such as HIV, Hepatitis B (HBV), and Hepatitis C (HCV) in donated blood — far earlier than conventional antibody tests. [S2]
The case squarely raises the intersection of Article 21 (Right to Life), public health infrastructure capacity, and federalism — a high-probability Prelims and Mains topic.
Currently, most Indian blood banks rely on ELISA (Enzyme-Linked Immunosorbent Assay), which cannot detect infections during the "window period" before antibodies develop. [S1]

2. Why in the News

On 3 March 2026, a Supreme Court Bench comprising Chief Justice Surya Kant, Justice Joymalya Bagchi, and Justice Vipul M. Pancholi heard a petition filed by NGO Sarvesham Mangalam Foundation, which sought mandatory NAT testing in all blood banks. [S1]
The Bench raised the critical question of cost-effectiveness and whether resource-constrained States could afford NAT in government hospitals. [S1]
The petitioner argued that safe blood transfusion is a fundamental right under Article 21 of the Constitution. [S1]
Court posted the case for further hearing on 13 March 2026 after asking the petitioner to file an affidavit detailing which States and how many hospitals currently use NAT. [S1]

3. Background & Evolution

Blood transfusion-transmitted infections (TTIs) — HIV, HBV, HCV — have been a longstanding public health concern in India.
India's blood safety framework has historically been governed by the Drugs and Cosmetics Act, 1940 and rules thereunder, with blood banks regulated by the Central Drugs Standard Control Organisation (CDSCO) under the Ministry of Health & Family Welfare.
ELISA became the gold standard for blood screening in India in the 1990s; however, ELISA cannot detect infections during the serological window period — the gap between infection and antibody formation.
NAT was developed globally to close this gap; it detects viral nucleic acids (RNA/DNA) directly, dramatically reducing the window period. [S2]
Madhya Pradesh implemented a Centralized NAT Model for blood donor screening — one of the early Indian state-level experiments in mandatory NAT. [S3]
A 15-year retrospective study from Indian blood banks found NAT detected 205 additional TTI cases missed by serology, with HBV accounting for the majority (79.76%) of NAT-only yields. [S2]
WHO has actively promoted NAT integration into national blood safety programs through its blood safety frameworks and webinar series for SEARO (South-East Asia Regional Office). [S4]

4. Core Static Facts

Parameter	Detail
Full form of NAT	Nucleic Acid Test (also called Nucleic Acid Amplification Test / NAAT)
What it detects	Viral genetic material — RNA (HIV, HCV) and DNA (HBV)
Comparator test	ELISA (Enzyme-Linked Immunosorbent Assay) — detects antibodies/antigens, not viral nucleic acid
Key advantage of NAT over ELISA	Closes the window period — phase where virus is present but antibodies undetectable
Window period reduction (NAT)	Reduces transfusion-transmitted infection risk to approximately 1 in a million [S2]
Viruses targeted	HIV, Hepatitis B Virus (HBV), Hepatitis C Virus (HCV)
Regulatory body (India)	Central Drugs Standard Control Organisation (CDSCO), under Ministry of Health & Family Welfare
Enabling legislation	Drugs and Cosmetics Act, 1940; Blood Bank Regulations under Schedule F, Part XII-B
Petitioner	NGO Sarvesham Mangalam Foundation
Bench	CJI Surya Kant + Justices Joymalya Bagchi + Vipul M. Pancholi
Constitutional peg	Article 21 — Right to Life (safe blood = right to life)
NAT yield split (Indian data)	HBV: 79.76% \| HCV: 16.83% \| HIV: 3.41% [S2]
State model	Madhya Pradesh — Centralized NAT Model [S3]

5. Multi-Dimensional Analysis

Scientific / Technological

NAT detects viral nucleic acids (RNA or DNA) directly, bypassing the need for antibody formation — this shrinks the serological window period from weeks to days. [S2]
Two main NAT platforms used globally: pooled NAT (tests multiple samples together — cost-effective) and individual donation NAT (ID-NAT) (higher sensitivity).
A 15-year Indian retrospective study demonstrates NAT's clinical utility: 205 TTI cases that would have entered the blood supply under ELISA-only screening were intercepted by NAT. [S2]
WHO SEARO has issued guidelines and conducted pilot webinar series on Quality Assurance in Transfusion Transmissible Infections (TTI) testing, promoting NAT adoption. [S4]

Legal / Constitutional

The petition frames blood safety as a component of the right to life under Article 21, following the SC's expansive jurisprudence (Paschim Banga Khet Mazdoor Samity, 1996 — State obligated to provide basic medical care).
If the SC mandates NAT, it would create a judicial directive binding all State governments — raising questions of federal fiscal autonomy (Entry 6, State List — public health is a State subject).
Any mandatory protocol will require amendment to Schedule F, Part XII-B of the Drugs and Cosmetics Rules, 1945 — a Central regulatory act.

Economic

The Bench itself raised the fiscal federalism concern: States struggling to pay salaries or electricity bills cannot easily absorb capital-intensive NAT infrastructure. [S1]
Pooled NAT can reduce per-unit cost significantly vs ID-NAT; Madhya Pradesh's centralized model demonstrates economies of scale. [S3]
Failure to adopt NAT imposes downstream economic costs via transfusion-transmitted HIV/HBV/HCV — lifelong treatment costs, productivity loss, legal liability.

Social / Equity

Patients requiring repeated transfusions — thalassemia patients, haemophiliacs, cancer patients — are disproportionately exposed to window-period risk; mandatory NAT would benefit these vulnerable groups most.
India has an estimated 1.5 lakh thalassemia major patients dependent on regular blood transfusions (approximated from disease burden data).
Rural and district-level blood banks in poorer States have least access to NAT technology — a health equity gap.

Administrative / Governance

Public health is a State subject (Entry 6, State List, Schedule VII) — Centre can set standards via CDSCO under the Drugs and Cosmetics Act but cannot directly compel States to fund NAT.
Implementation asymmetry: Maharashtra, Delhi, Tamil Nadu may be able to absorb NAT costs; BIMARU States and northeastern States face structural barriers.
Centralized regional NAT hubs (MP model) represent a viable governance innovation — pooling samples from multiple blood banks to one testing centre.

Ethical / Governance

There is a duty of care principle at stake: knowingly transfusing blood screened only by ELISA (when a superior technology exists) may constitute negligence.
Informed consent in blood transfusion contexts does not typically disclose test methodology — raising transparency concerns.

6. Recent Developments (Last 12–18 Months)

3 March 2026: SC Bench (CJI Surya Kant + 2 Justices) takes up petition by Sarvesham Mangalam Foundation; questions cost-effectiveness of NAT vs ELISA; asks States' data affidavit. [S1]
13 March 2026: Next hearing date set by SC for further consideration. [S1]
2025 (published): A 15-year retrospective study from Indian blood banks (published in a peer-reviewed journal) quantified NAT's added value — 205 additional TTI detections over ELISA-only screening. [S2]
Madhya Pradesh Centralized NAT Model published in peer-reviewed literature (2025–26), providing a replicable State-level template. [S3]
WHO SEARO's Quality Assurance webinar series (ongoing) promotes NAT standard-setting across South/South-East Asia. [S4]

7. Prelims Hooks

NAT stands for Nucleic Acid Test (also: Nucleic Acid Amplification Test / NAAT) — it detects viral genetic material, not antibodies.
NAT can detect HIV, Hepatitis B, and Hepatitis C viruses in donated blood.
ELISA (Enzyme-Linked Immunosorbent Assay) is the currently predominant blood-bank screening test in India — it detects antibodies/antigens, not nucleic acids.
The petitioner in the SC case is NGO Sarvesham Mangalam Foundation. [S1]
The Constitutional basis of the petition is Article 21 (Right to Life). [S1]
The SC Bench hearing this matter is headed by Chief Justice Surya Kant. [S1]
NAT reduces transfusion-transmitted infection risk to approximately 1 in a million. [S2]
In Indian blood bank data, HBV (Hepatitis B) accounts for the largest share (~80%) of infections detected by NAT but missed by ELISA. [S2]
Public health is a State subject under Entry 6, State List, Schedule VII of the Constitution — relevant to whether Centre can mandate NAT.
Blood banks in India are regulated under Schedule F, Part XII-B of the Drugs and Cosmetics Rules, 1945, administered by CDSCO.
The regulatory body overseeing blood banks is the Central Drugs Standard Control Organisation (CDSCO) under the Ministry of Health & Family Welfare.
Madhya Pradesh has piloted a Centralized NAT Model for blood donor screening. [S3]
The next SC hearing on NAT was posted for 13 March 2026. [S1]
The key distinction: NAT closes the serological window period — a phase where conventional antibody tests give a false-negative despite active infection.

8. Mains Relevance

GS Papers: - GS-II: Government policies and interventions for development in various sectors; health; SC/judiciary role; federalism; fundamental rights. - GS-III: Science and technology — applications and effects in everyday life; awareness in bio-technology.

Specific Syllabus Headings: - Issues relating to development and management of Social Sector / Services relating to Health. - Role of Judiciary in policy-making (judicial activism vs restraint). - Science & Technology — biotechnology / medical diagnostics.

Plausible Mains Questions:

"The Supreme Court's examination of mandatory Nucleic Acid Testing (NAT) in blood banks raises fundamental questions about the State's obligation under Article 21. Discuss the public health, legal, and fiscal dimensions of making NAT compulsory across India." (GS-II / GS-III)
"Critically examine the limitations of ELISA-based blood screening in India and evaluate how adoption of Nucleic Acid Testing (NAT) can address the residual risk of transfusion-transmitted infections. What governance model would best suit India's federal structure?" (GS-III)
"With public health being a State subject, how should the Centre ensure uniform blood safety standards, including advanced molecular screening technologies, across all States? Discuss with reference to the Drugs and Cosmetics Act framework." (GS-II)

9. Related Topics to Study Next

Topic	Connection
Drugs and Cosmetics Act, 1940 & CDSCO	Regulatory framework governing blood banks and any mandatory NAT notification
Article 21 and Right to Health jurisprudence	Constitutional basis; landmark SC judgments on health as part of right to life
National Blood Policy, 2002	India's overarching policy framework for safe blood — needs to be updated to include NAT mandate
ELISA & Serological Testing — Methodology	Prelims: understand how ELISA works to contrast with NAT; frequently confused
Federal Health Governance (State vs Central jurisdiction)	Entry 6 State List; concurrent list; Centre's role under Entry 26 for standards
Thalassemia & Haemophilia — Blood Disorder Burden in India	The population most at risk from inadequate transfusion screening
National AIDS Control Programme (NACP) & NACO	HIV prevention through blood safety is a NACP mandate — links to NAT policy
WHO Blood Safety Guidelines (SEARO)	International benchmarks India is compared against; WHO's role in norm-setting

10. Common Errors / Trap Areas

NAT vs NAAT vs PCR: Aspirants often conflate NAT with PCR specifically. NAT is the broader category (includes PCR, TMA — Transcription-Mediated Amplification, etc.); PCR is one NAT method.
Ministry confusion: Blood bank regulation falls under Ministry of Health & Family Welfare (via CDSCO), not the Ministry of Science & Technology or DBT — despite NAT being a biotech tool.
Constitutional List confusion: Public health is State List (Entry 6), but standards for drugs/blood products are regulated by the Centre under the Drugs and Cosmetics Act — a concurrent-type Central law. Do not say the Centre has no jurisdiction.
ELISA detects the virus directly — WRONG: ELISA detects antibodies or antigens, not viral genetic material. NAT detects the virus's genetic material directly. This is the most commonly tested distinction.
Assuming NAT replaces ELISA entirely: In most protocols, NAT is used alongside ELISA as an additional safety layer, not as a complete replacement — important for policy questions.

11. Sources

[S1] "SC to look into feasibility of NAT for blood transfusion" — The Hindu, 3 March 2026 (article excerpt provided as primary source, Tier 4) — https://www.thehindu.com/todays-paper/2026-03-03/th_international/articleGC7FLOM1P-13724494.ece
[S2] "Added Value of Nucleic Acid Testing in Blood Banks: A 15-Year Retrospective Study from India" — NCBI/PMC — https://www.ncbi.nlm.nih.gov/pmc/articles/PMC12776245/ (Tier 3)
[S3] "Blood Safety: The Madhya Pradesh Centralized Nucleic Acid Testing (NAT) Model for Blood Donor Screening" — NCBI/PMC — https://www.ncbi.nlm.nih.gov/pmc/articles/PMC12869267/ (Tier 3)
[S4] "Online Pilot Webinar Series on Quality Assurance in Transfusion Transmissible Infections Testing" — WHO SEARO — https://cdn.who.int/media/docs/default-source/searo/blt/online-pilot-webinar-series-on-quality-assurance-in-transfusion-transmissible-infections-testing_april_2021.pdf (Tier 2)