(Paper) Class - XII Sample Paper Biotechnology (Theory) 2008
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Class
- XII Sample Paper Biotechnology (Theory) 2008
Biotechnology
Sample Paper
(Theory)
Class - XII - (2008)
TIME:
3 HOUR
MARK: 70
GENERAL
INSTRUCTIONS:
a.
This question paper consists of four sections A, B, C and D. Section
A contains 5 questions of 1 mark each. Section B contains 10 questions of 2
marks each. Sections C contain 10 questions of 3 marks each and section D
contains 3 questions of 5 marks each.
b. All questions are compulsory.
c.
Question numbers 1 to 5 are very short answer type questions, carrying 1 mark
each.
d.
Question numbers 6 to 15 are short answer type questions, carrying 2 marks each.
e.
Question numbers 16 to 25 are also short answer type questions, carrying 3 mark
each.
f.
Question numbers 26 to 28 are long answer type questions, carrying 5 marks each.
SECTION
- A
1.
Write the names of two dyes used in two-dimensional gel electrophoresis
(1
2.
Why curd is used as pro-biotic? (1
3.
Define turbid state (1
5.
Name the plant from which agar is isolating
(1
SECTION
- B
6.
How does media helps to regulate pH in animal cell cultures? (2
7.
What is the role of curator in Bioinformatics data analysis?
(2
8.
How is calcium alginate useful in the rapid and mass propagation of elite
plant species? (2
9.
When irradiated with UV-light, yeast cultures express proteins involved
in DNA repair. Indicate Which library you would use to clone the genes for these
proteins? (2
10.
How the monoclonal antibodies are different from polyclonal antibodies?
Write one application of monoclonal antibodies in diagnosis
(2
11.
‘A particular Defence mechanism of bacteria is the basis of recombinant
DNA technology’. Explain (2
12.
Write four ethical issues of microbial technology
(2
13.
Write a short note on cosmids (2
14.
Give at least four steps can
be taken to maximize the protein stability during various isolation procedure
(2
15.
What are the advantages of using molecular markers over that of
morphological markers (2
SECTION
- C
Diagrammatically represent the steps of Southern
hybridization (3
16.
Write notes on
a) Micro-injection
b) Electroporation
c) Transformation (3
17.
Mr. Arvind sequenced the genome of an unknown organism. He wants to know
the ancestry of the organism and the homologous sequences. Guide him by giving
the procedure of the method (3
18. Explain three reasons why the use of microbes may be harmful in making product of human conception (3)
19.
Study the following enzyme purification table and answer the question
that follow
Step |
Procedure |
Total
protein (mg) |
Activity
(units) |
1 |
Crude
extract |
1200 |
2400 |
2 |
Precipitation(salt) |
300 |
2100 |
3 |
Ion
exchange chromatography |
150 |
1800 |
4 |
Gel
chromatography |
120 |
1600 |
5 |
Affinity
chromatography |
3 |
1200 |
a)
Which is the yield of active protein from crude extract?
b)
Which step in the purification is least effective. Why?
c)
Which step in the purification is most effective. Why?
(3
21. Write a note on edible vaccines
OR
Diagrammatically
differentiate dATP and ddATP (3
22.
Explain three reasons Why the use of microbes may be harmful in making products
of human consumption (3
23.
How can you obtain virus free potato plant from virus infected plants? Are these
plants virus resistant? Why or why not? (3
24.
Karyotype determination of established cell line is very important. Explain
(3
25.
Name the enzymes which known as ‘laundry enzymes’. How it is inactivated?
How can we increase the stability of the enzymes?
(3
SECTION
– D
26.
What is Proteomics? Explain different types of Proteomics with one
examples (5
OR
a)
Describe the important parts of mass spectrometer with the help of a suitable
diagram
b) Explain how proteins are volatilized as well as analysed by mass
spectrometer.
c)
Why has this technique become so important for biotechnology
(5
27.
What is PCR? What is its underlying principle? Explain the steps with the help
of suitable diagrams (5
28.
What is Proteomics? Explain different types of Proteomics with one example
(5
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